MedTrace Logo

Trial Outcomes & Findings for Study of Efficacy and Safety of NIS793 in Combination With Standard of Care (SOC) Chemotherapy in First-line Metastatic Pancreatic Ductal Adenocarcinoma (mPDAC) - daNIS-2 (NCT NCT04935359)

NCT ID: NCT04935359

Last Updated: 2026-05-19

Results Overview

A dose-limiting toxicity (DLT) was defined as an adverse event or abnormal laboratory value assessed as unrelated to disease, disease progression, inter-current illness, or concomitant medications that occurred within the first cycle (i.e., 28 days or 4 weeks) of the treatment with NIS793 in combination with gemcitabine/nab-paclitaxel. The National Cancer Institute Common Terminology Criteria for Adverse events (NCI CTCAE) version 5 was used for all grading.

Recruitment status

COMPLETED

Study phase

PHASE3

Target enrollment

511 participants

Primary outcome timeframe

Up to 4 weeks

Results posted on

2026-05-19

Participant Flow

The study was conducted globally across 27 countries.

Participant milestones

Participant milestones
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Overall Study
STARTED
21
245
245
Overall Study
Entered Post Treatment Follow-up
18
192
200
Overall Study
COMPLETED
0
0
0
Overall Study
NOT COMPLETED
21
245
245

Reasons for withdrawal

Reasons for withdrawal
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Overall Study
Progressive disease
17
148
149
Overall Study
Physician Decision
2
20
24
Overall Study
Adverse Event
1
25
24
Overall Study
Lost to Follow-up
1
0
0
Overall Study
Death
0
16
8
Overall Study
Guardian decision
0
1
0
Overall Study
Sponsor decision
0
9
16
Overall Study
Participant decision
0
25
24
Overall Study
Participants not treated due to Protocol deviation
0
1
0

Baseline Characteristics

Study of Efficacy and Safety of NIS793 in Combination With Standard of Care (SOC) Chemotherapy in First-line Metastatic Pancreatic Ductal Adenocarcinoma (mPDAC) - daNIS-2

Baseline characteristics by cohort

Baseline characteristics by cohort
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=21 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Total
n=511 Participants
Total of all reporting groups
Age, Customized
<= 65 years
13 Participants
n=30 Participants
130 Participants
n=30 Participants
125 Participants
n=60 Participants
268 Participants
n=133 Participants
Age, Customized
Between 65 and 75 years
7 Participants
n=30 Participants
97 Participants
n=30 Participants
91 Participants
n=60 Participants
195 Participants
n=133 Participants
Age, Customized
>= 75 years
1 Participants
n=30 Participants
18 Participants
n=30 Participants
29 Participants
n=60 Participants
48 Participants
n=133 Participants
Sex: Female, Male
Female
6 Participants
n=30 Participants
109 Participants
n=30 Participants
99 Participants
n=60 Participants
214 Participants
n=133 Participants
Sex: Female, Male
Male
15 Participants
n=30 Participants
136 Participants
n=30 Participants
146 Participants
n=60 Participants
297 Participants
n=133 Participants
Race (NIH/OMB)
American Indian or Alaska Native
0 Participants
n=30 Participants
3 Participants
n=30 Participants
0 Participants
n=60 Participants
3 Participants
n=133 Participants
Race (NIH/OMB)
Asian
2 Participants
n=30 Participants
87 Participants
n=30 Participants
87 Participants
n=60 Participants
176 Participants
n=133 Participants
Race (NIH/OMB)
Native Hawaiian or Other Pacific Islander
0 Participants
n=30 Participants
1 Participants
n=30 Participants
0 Participants
n=60 Participants
1 Participants
n=133 Participants
Race (NIH/OMB)
Black or African American
0 Participants
n=30 Participants
9 Participants
n=30 Participants
6 Participants
n=60 Participants
15 Participants
n=133 Participants
Race (NIH/OMB)
White
19 Participants
n=30 Participants
137 Participants
n=30 Participants
143 Participants
n=60 Participants
299 Participants
n=133 Participants
Race (NIH/OMB)
More than one race
0 Participants
n=30 Participants
1 Participants
n=30 Participants
0 Participants
n=60 Participants
1 Participants
n=133 Participants
Race (NIH/OMB)
Unknown or Not Reported
0 Participants
n=30 Participants
7 Participants
n=30 Participants
9 Participants
n=60 Participants
16 Participants
n=133 Participants

PRIMARY outcome

Timeframe: Up to 4 weeks

Population: Dose-Determining Set (DDS) - The DDS consisted of all participants in the safety run-in part who met the minimum exposure criterion and had sufficient safety evaluations after 4 weeks of treatment or experienced a DLT during the first 4 weeks of treatment.

A dose-limiting toxicity (DLT) was defined as an adverse event or abnormal laboratory value assessed as unrelated to disease, disease progression, inter-current illness, or concomitant medications that occurred within the first cycle (i.e., 28 days or 4 weeks) of the treatment with NIS793 in combination with gemcitabine/nab-paclitaxel. The National Cancer Institute Common Terminology Criteria for Adverse events (NCI CTCAE) version 5 was used for all grading.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=18 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Safety run-in Part: Percentage of Participants With Dose Limiting Toxicities (DLTs) During the First Cycle (4 Weeks) of Treatment.
0 Participants

PRIMARY outcome

Timeframe: From randomization up to death, assessed up to approximately 34 months

Population: The Full Analysis Set (FAS) in the Randomized Part included all participants assigned study treatment by randomization and were analyzed according to the treatment they were assigned during the randomization procedure.

Overall Survival (OS) was defined as the time from date of randomization/start of treatment to date of death due to any cause. If a patient was not known to have died, survival was censored at the date of last known date patient alive.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part: Overall Survival (OS)
9.2 Months
Interval 8.1 to 10.5
11.2 Months
Interval 9.6 to 12.1

SECONDARY outcome

Timeframe: Up to approximately 32 months

Population: The Safety Set (SAF) in the Run-in part included all participants who received at least one dose of study treatment, including incomplete infusions, and were analyzed according to the treatment(s) they received. In the Randomized Part, the SAF included all participants who received at least one dose of study treatment, including incomplete infusions, and were analyzed according to the treatment they received, either the randomized treatment assigned or the first treatment received.

An adverse event (AE) is any untoward medical occurrence (e.g. any unfavorable and unintended sign \[including abnormal laboratory findings\], symptom or disease) in a clinical investigation participant after providing written informed consent for participation in the study. Therefore, an AE may or may not be temporally or causally associated with the use of a medicinal (investigational) product. Treatment emergent Adverse Event (TEAEs) in this study are events that started after the first dose of study treatment and until 30 days after last dose of SOC chemotherapies and up to 90 days after NIS793, whichever is later.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=21 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=239 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=241 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Percentage of Participants With Adverse Events (AEs)
Adverse Events (AEs)
21 Participants
239 Participants
239 Participants
Percentage of Participants With Adverse Events (AEs)
Serious Adverse Events (SAEs)
13 Participants
144 Participants
110 Participants
Percentage of Participants With Adverse Events (AEs)
Fatal SAEs
0 Participants
12 Participants
8 Participants
Percentage of Participants With Adverse Events (AEs)
AEs leading to discontinuation
2 Participants
46 Participants
50 Participants
Percentage of Participants With Adverse Events (AEs)
AEs leading to dose adjustment/interruption
16 Participants
205 Participants
208 Participants
Percentage of Participants With Adverse Events (AEs)
AEs requiring additional therapy
21 Participants
231 Participants
227 Participants

SECONDARY outcome

Timeframe: Up to approximately 32 months

Population: The Safety Set (SAF) in the Run-in part included all participants who received at least one dose of study treatment, including incomplete infusions, and were analyzed according to the treatment(s) they received. In the Randomized Part, the SAF included all participants who received at least one dose of study treatment, including incomplete infusions, and were analyzed according to the treatment they received, either the randomized treatment assigned or the first treatment received.

No dose reductions were allowed for NIS793 in the Randomized part and beyond the first 28 days period of the Safety Run-in part. Increasing the dosing interval from every 2 weeks (Q2W) to every 2 weeks (Q4W) was allowed. Dose interruption for NIS793 was permitted if adverse drug reaction was suspected to be related to NIS793. If NIS793 was interrupted or delayed for \> 8 weeks due to toxicity that was suspected to be related to treatment, study treatment was permanently discontinued.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=21 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=239 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=241 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Percentage of Participants With Dose Interruptions and Dose Reductions of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
With no dose interruption
5 Participants
92 Participants
82 Participants
Percentage of Participants With Dose Interruptions and Dose Reductions of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
With at least one dose interruption
16 Participants
147 Participants
159 Participants
Percentage of Participants With Dose Interruptions and Dose Reductions of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
With at least one dose reduction
0 Participants
2 Participants
0 Participants
Percentage of Participants With Dose Interruptions and Dose Reductions of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
With no dose reduction
21 Participants
237 Participants
241 Participants

SECONDARY outcome

Timeframe: Up to approximately 32 months

Population: The Safety Set (SAF) in the Run-in part included all participants who received at least one dose of study treatment, including incomplete infusions, and were analyzed according to the treatment(s) they received. In the Randomized Part, the SAF included all participants who received at least one dose of study treatment, including incomplete infusions, and were analyzed according to the treatment they received, either the randomized treatment assigned or the first treatment received.

Dose intensity was computed as the ratio of actual cumulative dose received and actual duration of exposure.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=21 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=239 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=241 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Dose Intensity of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
3669.2 mg/cycle
Standard Deviation 528.07
3134.1 mg/cycle
Standard Deviation 573.15
3183.4 mg/cycle
Standard Deviation 593.92

SECONDARY outcome

Timeframe: From enrollment (run-in part) or randomization (randomized part) up to disease progression or death, assessed up to approximately 34 months

Population: The Full Analysis Set (FAS) in the Safety Run-in Part included all participants who received any study drug and were analyzed according to the treatment(s) received, following the intent-to-treat (ITT) principle. In the Randomized Part, the FAS included all participants assigned study treatment by randomization and were analyzed according to the treatment they were assigned during the randomization procedure.

Progression-Free Survival (PFS) was defined as the time from the enrollment (run-in part) or randomization (randomized part) to the date of the first documented disease progression based on local investigator assessment as per RECIST 1.1 or date of death due to any cause, whichever occurs first. PFS was censored if no PFS event was observed before the analysis cut-off date. The censoring date was the date of the last adequate tumor assessment prior to the analysis cut-off.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=21 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Progression-Free Survival (PFS)
5.4 Months
Interval 3.6 to 7.3
4.6 Months
Interval 3.7 to 5.4
5.4 Months
Interval 5.3 to 6.6

SECONDARY outcome

Timeframe: Up to approximately 34 months

Population: The Full Analysis Set (FAS) in the Safety Run-in Part included all participants who received any study drug and were analyzed according to the treatment(s) received, following the intent-to-treat (ITT) principle. In the Randomized Part, the FAS included all participants assigned study treatment by randomization and were analyzed according to the treatment they were assigned during the randomization procedure.

Overall Response Rate (ORR) was defined as the proportion of participants with a Best Overall Response (BOR) of Complete Response (CR) or Partial Response (PR) as per local review. ORR was evaluated according to RECIST 1.1. The BOR was determined from response assessments undertaken while on treatment.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=21 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Overall Response Rate (ORR)
19.0 Percentage of participants
Interval 5.4 to 41.9
21.6 Percentage of participants
Interval 16.6 to 27.3
25.3 Percentage of participants
Interval 20.0 to 31.2

SECONDARY outcome

Timeframe: Up to approximately 34 months

Population: The Full Analysis Set (FAS) in the Safety Run-in Part included all participants who received any study drug and were analyzed according to the treatment(s) received, following the intent-to-treat (ITT) principle. In the Randomized Part, the FAS included all participants assigned study treatment by randomization and were analyzed according to the treatment they were assigned during the randomization procedure.

Disease Control Rate (DCR) was defined as the proportion of participants with Best Overall Response (BOR) of Complete Response (CR) or Partial Response (PR), or Stable Disease (SD) or Non-CR/Non-progressive disease as per local review. DCR was evaluated according to RECIST 1.1.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=21 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Disease Control Rate (DCR)
76.2 Percentage of participants
Interval 52.8 to 91.8
66.9 Percentage of participants
Interval 60.7 to 72.8
72.2 Percentage of participants
Interval 66.2 to 77.8

SECONDARY outcome

Timeframe: Up to approximately 34 months

Population: Full Analysis Set (FAS) - Only participants with first documented response (CR or PR) included

Duration of Response (DOR) was defined as the duration of time between the date of first documented response (CR or PR) and the date of first documented progression or death due to any cause.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=4 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=53 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=62 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Duration of Response (DOR)
8.6 Months
Interval 3.5 to
NA: Not estimable due to insufficient number of participants with events
6.2 Months
Interval 4.7 to 7.4
5.6 Months
Interval 5.0 to 7.2

SECONDARY outcome

Timeframe: From enrollment (run-in part) or randomization (randomized part) up to first documented response, assessed up to approximately 34 months

Population: The Full Analysis Set (FAS) in the Safety Run-in Part included all participants who received any study drug and were analyzed according to the treatment(s) received, following the intent-to-treat (ITT) principle. In the Randomized Part, the FAS included all participants assigned study treatment by randomization and were analyzed according to the treatment they were assigned during the randomization procedure.

Time to Response (TTR) was defined as the duration of time between the date of enrollment (run-in part) or randomization (randomized part) and the date of first documented response of either CR or PR as per local review, which was subsequently confirmed. TTR was evaluated according to RECIST 1.1. Participants without a confirmed CR or PR were censored at the time of PFS event (i.e., disease progression or death due to any cause) for participants with a PFS event (i.e., disease progression or death due to any cause), or at the date of the last adequate tumor assessment for participants without a PFS event.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=21 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
n=245 Participants
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Time to Response (TTR)
NA Months
NA: Not estimable due to number of events censored
NA Months
NA: Not estimable due to number of events censored
NA Months
NA: Not estimable due to number of events censored

SECONDARY outcome

Timeframe: Cycles 1 and 3 Day 15 (0 hour (pre-dose)), Cycles 2, 4, 6 and 12 Day 1 (0 hour (pre-dose)). 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Participants with corresponding evaluable PK parameters at the indicated timepoint were analyzed

Venous whole blood samples were collected for activity-based pharmacokinetics characterization. Ctrough was listed and summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=19 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Safety run-in Part: Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 4 Day 1
370000 ng/mL
Standard Deviation 148000
Safety run-in Part: Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 1 Day 15
230000 ng/mL
Standard Deviation 250000
Safety run-in Part: Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 2 Day 1
207000 ng/mL
Standard Deviation 82400
Safety run-in Part: Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1
300000 ng/mL
Standard Deviation 123000
Safety run-in Part: Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 15
309000 ng/mL
Standard Deviation 130000
Safety run-in Part: Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 6 Day 1
425000 ng/mL
Standard Deviation 86800
Safety run-in Part: Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 12 Day 1
553000 ng/mL
Standard Deviation NA
NA: Not estimable due to insufficient number of participants with events

SECONDARY outcome

Timeframe: Cycles 1 and 3 Day 1: 0 hour (pre-dose) and 1 hour. 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Participants with corresponding evaluable PK parameters at the indicated timepoint were analyzed

Venous whole blood samples were collected for activity-based pharmacokinetics characterization. Cmax was listed and summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=17 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Safety run-in Part: Maximum Concentration (Cmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 1 Day 1
549000 ng/mL
Standard Deviation 193000
Safety run-in Part: Maximum Concentration (Cmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1
837000 ng/mL
Standard Deviation 394000

SECONDARY outcome

Timeframe: Cycles 1 and 3 Day 1: 0 hour (pre-dose) and 1 hour. 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Participants with corresponding evaluable PK parameters at the indicated timepoint were analyzed

Venous whole blood samples were collected for activity-based pharmacokinetics characterization. Tmax was listed and summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=17 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Safety run-in Part: Time to Reach Maximum Concentration (Tmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 1 Day 1
1.12 Hour
Interval 0.583 to 5.0
Safety run-in Part: Time to Reach Maximum Concentration (Tmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1
0.883 Hour
Interval 0.5 to 4.17

SECONDARY outcome

Timeframe: Cycle 1 Day 15, Cycle 3 Day 1, Cycle 3 Day 15, Cycle 4 Day 1 and Cycle 6 Day 1: 0 hour (pre-dose). 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Chinese participants with intensive PK sampling with corresponding evaluable PK parameters at the indicated timepoint were analyzed

In the randomized part, participants enrolled for treatment in China were assigned to more intensive PK sampling (taken into account the ability of clinical sites to comply with the instructions in the laboratory manual concerning the preparation of serum samples) to assess PK of NIS793 in Chinese participants. Venous whole blood samples were collected for activity-based pharmacokinetics characterization and Ctrough was summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=20 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Chinese Participants With Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 1 Day 15: 0 hour (pre-dose)
149000 ng/mL
Standard Deviation 36400
Randomized Part (Chinese Participants With Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1: 0 hour (pre-dose)
366000 ng/mL
Standard Deviation 114000
Randomized Part (Chinese Participants With Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 15: 0 hour (pre-dose)
380000 ng/mL
Standard Deviation 187000
Randomized Part (Chinese Participants With Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 4 Day 1: 0 hour (pre-dose)
371000 ng/mL
Standard Deviation 131000
Randomized Part (Chinese Participants With Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 6 Day 1: 0 hour (pre-dose)
493000 ng/mL
Standard Deviation 221000

SECONDARY outcome

Timeframe: Cycles 1 and 3 Day 1: 0 hour (pre-dose) and 1 hour. 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Chinese participants with intensive PK sampling with corresponding evaluable PK parameters at the indicated timepoint were analyzed

In the randomized part, participants enrolled for treatment in China were assigned to more intensive PK sampling (taken into account the ability of clinical sites to comply with the instructions in the laboratory manual concerning the preparation of serum samples) to assess PK of NIS793 in Chinese participants. Venous whole blood samples were collected for activity-based pharmacokinetics characterization and Cmax was summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=23 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Chinese Participants With Intensive PK Sampling): Maximum Concentration (Cmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 1 Day 1
691000 ng/mL
Standard Deviation 113000
Randomized Part (Chinese Participants With Intensive PK Sampling): Maximum Concentration (Cmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1
978000 ng/mL
Standard Deviation 131000

SECONDARY outcome

Timeframe: Cycles 1 and 3 Day 1: 0 hour (pre-dose) and 1 hour. 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Chinese participants with intensive PK sampling with corresponding evaluable PK parameters at the indicated timepoint were analyzed

In the randomized part, participants enrolled for treatment in China were assigned to more intensive PK sampling (taken into account the ability of clinical sites to comply with the instructions in the laboratory manual concerning the preparation of serum samples) to assess PK of NIS793 in Chinese participants. Venous whole blood samples were collected for activity-based pharmacokinetics characterization and Tmax was summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=23 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Chinese Participants With Intensive PK Sampling): Time to Reach Maximum Concentration (Tmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 1 Day 1
1.52 Hour
Interval 0.583 to 7.0
Randomized Part (Chinese Participants With Intensive PK Sampling): Time to Reach Maximum Concentration (Tmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1
3.98 Hour
Interval 0.567 to 7.75

SECONDARY outcome

Timeframe: Cycles 1 Day 1: 0 hour (pre-dose) and 1 hour. 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Chinese participants with intensive PK sampling with corresponding evaluable PK parameters

In the randomized part, participants enrolled for treatment in China were assigned to more intensive PK sampling (taken into account the ability of clinical sites to comply with the instructions in the laboratory manual concerning the preparation of serum samples) to assess PK of NIS793 in Chinese participants. Venous whole blood samples were collected for activity-based pharmacokinetics characterization and AUClast was summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=23 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Chinese Participants With Intensive PK Sampling): Area Under the Curve From Time Zero to the Last Measurable Concentration Sampling Time (AUClast) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
48900000 h*ng/mL
Geometric Coefficient of Variation 104.3

SECONDARY outcome

Timeframe: Cycles 3 Day 1: 0 hour (pre-dose) and 1 hour. 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Chinese participants with intensive PK sampling with corresponding evaluable PK parameters

In the randomized part, participants enrolled for treatment in China were assigned to more intensive PK sampling (taken into account the ability of clinical sites to comply with the instructions in the laboratory manual concerning the preparation of serum samples) to assess PK of NIS793 in Chinese participants. Venous whole blood samples were collected and AUCtau was summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=7 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Chinese Participants With Intensive PK Sampling): Area Under the Curve Calculated to the End of a Dosing Interval (Tau) at Steady-state (AUCtau) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
159000000 h*ng/mL
Geometric Coefficient of Variation 25.5

SECONDARY outcome

Timeframe: Cycles 2, 3, 4, 6 and 12 Day 1 (0 hour (pre-dose)). 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Participants without intensive PK sampling with corresponding evaluable PK parameters at the indicated timepoint were analyzed

For participants without intensive PK sampling, venous whole blood samples were collected for activity-based pharmacokinetics characterization. Ctrough was listed and summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=129 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Participants Without Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 12 Day 1: 0 hour (pre-dose)
302000 ng/mL
Standard Deviation 63600
Randomized Part (Participants Without Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 2 Day 1: 0 hour (pre-dose)
249000 ng/mL
Standard Deviation 105000
Randomized Part (Participants Without Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1: 0 hour (pre-dose)
331000 ng/mL
Standard Deviation 133000
Randomized Part (Participants Without Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 4 Day 1: 0 hour (pre-dose)
335000 ng/mL
Standard Deviation 138000
Randomized Part (Participants Without Intensive PK Sampling): Trough Concentration (Ctrough) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 6 Day 1: 0 hour (pre-dose)
334000 ng/mL
Standard Deviation 136000

SECONDARY outcome

Timeframe: Cycles 1 and 3: Day 1 (0 hour (pre-dose)). 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Participants without intensive PK sampling with corresponding evaluable PK parameters at the indicated timepoint were analyzed

For Chinese participants without intensive PK sampling schedule and global participants in the randomized part, for which only sparse PK samples were collected for activity-based pharmacokinetics characterization, Cmax was listed and summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=152 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Participants Without Intensive PK Sampling): Maximum Concentration (Cmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 1 Day 1: 0 hour (pre-dose)
625000 ng/mL
Standard Deviation 185000
Randomized Part (Participants Without Intensive PK Sampling): Maximum Concentration (Cmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1: 0 hour (pre-dose)
807000 ng/mL
Standard Deviation 228000

SECONDARY outcome

Timeframe: Cycles 1 and 3: Day 1 (0 hour (pre-dose)). 1 cycle = 28 days.

Population: Pharmacokinetic Analysis Set - Participants without intensive PK sampling with corresponding evaluable PK parameters at the indicated timepoint were analyzed

For Chinese participants without intensive PK sampling schedule and global participants in the randomized part, for which only sparse PK samples were collected for activity-based pharmacokinetics characterization, Tmax was listed and summarized using descriptive statistics.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=152 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Participants Without Intensive PK Sampling): Time to Reach Maximum Concentration (Tmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 1 Day 1: 0 hour (pre-dose)
1.08 Hour
Interval 0.5 to 5.17
Randomized Part (Participants Without Intensive PK Sampling): Time to Reach Maximum Concentration (Tmax) of NIS793 in Combination With Gemcitabine and Nab-paclitaxel
Cycle 3 Day 1: 0 hour (pre-dose)
0.833 Hour
Interval 0.5 to 2.83

SECONDARY outcome

Timeframe: Baseline

Population: For the randomized part, the immunogenicity (IG) incidence set included all participants in the IG prevalence set with a determinant baseline IG sample.

Anti-drug antibodies (ADA) against NIS793 prevalence at baseline refers to the proportion of subjects who have developed antibodies against the drug NIS793 before starting treatment. This is calculated by dividing the number of subjects with ADA-positive samples at baseline by the total number of subjects whose baseline samples were tested for ADA.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=196 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part: Anti-drug Antibodies (ADA) Against NIS793 Prevalence at Baseline
ADA-negative sample at baseline
196 Participants
Randomized Part: Anti-drug Antibodies (ADA) Against NIS793 Prevalence at Baseline
ADA-positive sample at baseline
0 Participants

SECONDARY outcome

Timeframe: From date of first study drug intake up to approximately 34 months

Population: For the randomized part, the immunogenicity (IG) incidence set included all participants in the IG prevalence set with a determinant baseline IG sample and at least one determinant post-baseline IG sample.

Anti-drug antibodies (ADA) against NIS793 incidence on treatment refers to the proportion of participants who developed antibodies against the drug NIS793 during the treatment period. This can be categorized into two types: 1. Treatment-induced ADA positive: Participants who were ADA-negative at baseline but became ADA-positive after starting the treatment. 2. Treatment-boosted ADA positive: Participants who were ADA-positive at baseline and showed a significant increase in ADA titer during the treatment.

Outcome measures

Outcome measures
Measure
Safety run-in Part: NIS793 Plus (Gemcitabine and Nab-paclitaxel)
n=196 Participants
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel : * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm A): NIS793 Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of NIS793, Gemcitabine and Nab-paclitaxel: * NIS793 at 2100 mg (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part (Arm B): Placebo Plus (Gemcitabine and Nab-paclitaxel)
Participants received a combination of placebo, gemcitabine and nab-paclitaxel: * Placebo for NIS793 (Days 1 and 15) * Gemcitabine at 1000 mg/m² (Days 1, 8 and 15) * Nab-paclitaxel at 125 mg/m² (Days 1, 8 and 15)
Randomized Part: Anti-drug Antibodies (ADA) Against NIS793 Incidence on Treatment
Treatment-boosted ADA-positive
0 Participants
Randomized Part: Anti-drug Antibodies (ADA) Against NIS793 Incidence on Treatment
Treatment-induced ADA-positive
0 Participants
Randomized Part: Anti-drug Antibodies (ADA) Against NIS793 Incidence on Treatment
ADA-negative
196 Participants

Adverse Events

Safety Run-in (NIS793 + Gemcitabine/Nab-Paclitaxel): on-Treatment

Serious events: 13 serious events
Other events: 21 other events
Deaths: 0 deaths

Safety Run-in (NIS793 + Gemcitabine/Nab-Paclitaxel): Post-Treatment

Serious events: 2 serious events
Other events: 6 other events
Deaths: 19 deaths

Randomized Arm A (NIS793 + Gemcitabine/Nab-Paclitaxel): On-treatment

Serious events: 144 serious events
Other events: 228 other events
Deaths: 24 deaths

Randomized Arm A (NIS793 + Gemcitabine/Nab-Paclitaxel): Post-treatment

Serious events: 21 serious events
Other events: 29 other events
Deaths: 135 deaths

Randomized Arm B (Placebo + Gemcitabine/Nab-Paclitaxel): On-Treatment

Serious events: 110 serious events
Other events: 236 other events
Deaths: 16 deaths

Randomized Arm B (Placebo + Gemcitabine/Nab-Paclitaxel): Post-Treatment

Serious events: 28 serious events
Other events: 36 other events
Deaths: 132 deaths

Serious adverse events

Serious adverse events
Measure
Safety Run-in (NIS793 + Gemcitabine/Nab-Paclitaxel): on-Treatment
n=21 participants at risk
Safety run-in (NIS793 + gemcitabine/nab-paclitaxel): Events up to 30 days safety follow-up
Safety Run-in (NIS793 + Gemcitabine/Nab-Paclitaxel): Post-Treatment
n=18 participants at risk
Safety run-in (NIS793 + gemcitabine/nab-paclitaxel): Events in the post-treatment follow-up phase
Randomized Arm A (NIS793 + Gemcitabine/Nab-Paclitaxel): On-treatment
n=239 participants at risk
Randomized Arm A (NIS793 + gemcitabine/nab-paclitaxel): Events up to 30 days safety follow-up
Randomized Arm A (NIS793 + Gemcitabine/Nab-Paclitaxel): Post-treatment
n=192 participants at risk
Randomized Arm A (NIS793 + gemcitabine/nab-paclitaxel): Events in the post-treatment follow-up phase
Randomized Arm B (Placebo + Gemcitabine/Nab-Paclitaxel): On-Treatment
n=241 participants at risk
Randomized Arm B (Placebo + gemcitabine/nab-paclitaxel): Events up to 30 days safety follow-up
Randomized Arm B (Placebo + Gemcitabine/Nab-Paclitaxel): Post-Treatment
n=200 participants at risk
Randomized Arm B (Placebo + gemcitabine/nab-paclitaxel): Events in the post-treatment follow-up phase
Blood and lymphatic system disorders
Anaemia
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.4%
13/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Atypical haemolytic uraemic syndrome
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Blood loss anaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.6%
1/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Coagulopathy
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Disseminated intravascular coagulation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Febrile neutropenia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Leukocytosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Neutropenia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Pancytopenia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Thrombotic microangiopathy
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Acute myocardial infarction
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Atrial fibrillation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Cardiac arrest
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Cardiac disorder
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Cardiac failure
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Cardiac valve disease
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Cardiopulmonary failure
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Coronary artery disease
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Heart failure with preserved ejection fraction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Myocardial infarction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Palpitations
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Cardiac disorders
Ventricular fibrillation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Intestinal obstruction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Ischaemic enteritis
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Large intestinal obstruction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Lower gastrointestinal haemorrhage
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Malignant ascites
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Malignant gastrointestinal obstruction
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Melaena
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Obstruction gastric
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Pancreatitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Pancreatitis acute
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Portal hypertensive gastropathy
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Rectal haemorrhage
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Small intestinal haemorrhage
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Small intestinal obstruction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Small intestinal perforation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Upper gastrointestinal haemorrhage
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.3%
8/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Vomiting
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
5/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Asthenia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Condition aggravated
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Death
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Fatigue
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
General physical health deterioration
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.5%
6/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.6%
3/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Generalised oedema
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Malaise
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Oedema peripheral
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Pain
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Pyrexia
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
4.6%
11/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
4.6%
11/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Cholangitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.9%
7/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.5%
6/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Autoimmune hepatitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Bile duct stenosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Biliary obstruction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
5/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Cholangitis acute
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Cholecystitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Cholecystitis acute
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Gallbladder fistula
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Hepatic function abnormal
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Hepatobiliary disease
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Jaundice
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Jaundice cholestatic
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Liver disorder
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Malignant biliary obstruction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Hepatobiliary disorders
Portal vein thrombosis
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Abdominal abscess
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Abdominal infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Anal abscess
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Appendicitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Bacteraemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Bacterial infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Biliary tract infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
5/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
COVID-19
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
COVID-19 pneumonia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Cellulitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Cholangitis infective
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Clostridium difficile colitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Clostridium difficile infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Device related infection
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Device related sepsis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Erysipelas
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Escherichia infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Escherichia sepsis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Escherichia urinary tract infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.6%
1/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Eye infection
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Febrile infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Focal peritonitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Gastroenteritis
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Giardiasis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Hepatic infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Liver abscess
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Lower respiratory tract infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Nail infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Oesophageal candidiasis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Oral candidiasis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Oropharyngitis fungal
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Pancreas infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Penile infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Peritonitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Pneumococcal infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Pneumonia
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.9%
7/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.9%
7/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Pneumonia bacterial
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Pyelonephritis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Rhinovirus infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Sepsis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
5/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.9%
7/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Septic shock
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
5/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Sinusitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Urinary tract infection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Urosepsis
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Anastomotic ulcer
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Fall
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Femur fracture
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Fractured sacrum
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Hepatic rupture
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Hip fracture
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Infusion related reaction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Spinal fracture
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Vascular pseudoaneurysm ruptured
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Injury, poisoning and procedural complications
Wound dehiscence
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Alanine aminotransferase increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Amylase increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Aspartate aminotransferase increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Blood alkaline phosphatase increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Blood bilirubin increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Blood creatinine increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Lipase increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Platelet count decreased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Troponin increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Weight decreased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
White blood cell count decreased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Decreased appetite
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Dehydration
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Diabetic ketoacidosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Failure to thrive
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypercalcaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hyperglycaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hyperkalaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypoalbuminaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypoglycaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypokalaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hyponatraemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypophosphataemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Malnutrition
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Metabolic acidosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Back pain
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Muscular weakness
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Myalgia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Osteoporotic fracture
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Pain in extremity
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Pathological fracture
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Sarcopenia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
Oesophageal adenocarcinoma
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
Transitional cell carcinoma
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
Tumour associated fever
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
Tumour haemorrhage
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Cerebral haemorrhage
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Cerebral infarction
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Cerebrovascular accident
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Coma
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Dizziness
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Dysstasia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Encephalopathy
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Facial paralysis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Haemorrhage intracranial
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Headache
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Ischaemic stroke
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Metabolic encephalopathy
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Motor dysfunction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Neuropathy peripheral
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Neurotoxicity
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Putamen haemorrhage
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Seizure
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Syncope
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Transient ischaemic attack
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Product Issues
Device dislocation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Product Issues
Device occlusion
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Product Issues
Stent malfunction
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Psychiatric disorders
Delirium
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Renal and urinary disorders
Acute kidney injury
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Renal and urinary disorders
Calculus urinary
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Renal and urinary disorders
Haematuria
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Renal and urinary disorders
Hydronephrosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Renal and urinary disorders
Nephrolithiasis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Renal and urinary disorders
Renal failure
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Dyspnoea
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Epistaxis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Haemoptysis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Hiccups
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Hydrothorax
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Hypoxia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Interstitial lung disease
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Non-cardiogenic pulmonary oedema
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Pleural effusion
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Pneumonitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Pneumothorax
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Pulmonary embolism
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Respiratory distress
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Respiratory failure
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Skin and subcutaneous tissue disorders
Rash
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Aortic dissection
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Deep vein thrombosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Distributive shock
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Embolism
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.6%
1/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Hypotension
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Orthostatic hypotension
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Peripheral vein thrombosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Shock haemorrhagic
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Thrombophlebitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Eye disorders
Papilloedema
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Eye disorders
Retinal ischaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Eye disorders
Retinal vasculitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Abdominal distension
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Abdominal pain
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.3%
8/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Abdominal pain lower
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Abdominal pain upper
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Acute abdomen
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Ascites
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Colitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Constipation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Diarrhoea
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.5%
6/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Duodenal obstruction
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Duodenal stenosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Duodenal ulcer
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Dysphagia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Gastric haemorrhage
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Gastric perforation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Gastric stenosis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Gastrointestinal haemorrhage
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Gastrointestinal inflammation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.41%
1/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Gastrointestinal toxicity
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Gastrooesophageal reflux disease
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Haematemesis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Haematochezia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Haemorrhoidal haemorrhage
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Ileus
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.84%
2/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Impaired gastric emptying
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.

Other adverse events

Other adverse events
Measure
Safety Run-in (NIS793 + Gemcitabine/Nab-Paclitaxel): on-Treatment
n=21 participants at risk
Safety run-in (NIS793 + gemcitabine/nab-paclitaxel): Events up to 30 days safety follow-up
Safety Run-in (NIS793 + Gemcitabine/Nab-Paclitaxel): Post-Treatment
n=18 participants at risk
Safety run-in (NIS793 + gemcitabine/nab-paclitaxel): Events in the post-treatment follow-up phase
Randomized Arm A (NIS793 + Gemcitabine/Nab-Paclitaxel): On-treatment
n=239 participants at risk
Randomized Arm A (NIS793 + gemcitabine/nab-paclitaxel): Events up to 30 days safety follow-up
Randomized Arm A (NIS793 + Gemcitabine/Nab-Paclitaxel): Post-treatment
n=192 participants at risk
Randomized Arm A (NIS793 + gemcitabine/nab-paclitaxel): Events in the post-treatment follow-up phase
Randomized Arm B (Placebo + Gemcitabine/Nab-Paclitaxel): On-Treatment
n=241 participants at risk
Randomized Arm B (Placebo + gemcitabine/nab-paclitaxel): Events up to 30 days safety follow-up
Randomized Arm B (Placebo + Gemcitabine/Nab-Paclitaxel): Post-Treatment
n=200 participants at risk
Randomized Arm B (Placebo + gemcitabine/nab-paclitaxel): Events in the post-treatment follow-up phase
Blood and lymphatic system disorders
Anaemia
66.7%
14/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
69.0%
165/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.3%
16/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
59.3%
143/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.0%
10/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Leukopenia
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
6.3%
15/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
12.0%
29/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Neutropenia
23.8%
5/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
20.5%
49/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
27.4%
66/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Blood and lymphatic system disorders
Thrombocytopenia
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
15.1%
36/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
13.3%
32/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Abdominal distension
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.8%
9/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.9%
7/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Abdominal pain
38.1%
8/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.6%
1/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
10.5%
25/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
11.6%
28/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Abdominal pain upper
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.4%
13/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.0%
12/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Constipation
33.3%
7/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
19.7%
47/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
23.7%
57/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Diarrhoea
42.9%
9/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.6%
1/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
29.3%
70/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
33.2%
80/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Gingival bleeding
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.8%
9/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Haemorrhoids
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.9%
14/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Mouth ulceration
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
5/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Nausea
57.1%
12/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
37.2%
89/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
35.7%
86/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.5%
5/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Rectal haemorrhage
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.3%
8/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.2%
3/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Stomatitis
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
10.5%
25/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.3%
8/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Gastrointestinal disorders
Vomiting
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
23.8%
57/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
22.0%
53/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Asthenia
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
16.3%
39/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
18.7%
45/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.0%
4/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Chills
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.4%
13/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.4%
13/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Fatigue
57.1%
12/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
31.8%
76/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
32.4%
78/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.5%
5/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Malaise
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.8%
21/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
6.2%
15/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Oedema peripheral
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
15.1%
36/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
27.4%
66/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.5%
3/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Mucosal inflammation
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
4.6%
11/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.4%
13/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
General disorders
Pyrexia
23.8%
5/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.6%
1/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
31.4%
75/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
26.1%
63/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.5%
3/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
COVID-19
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.4%
20/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
9.5%
23/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Infections and infestations
Urinary tract infection
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
11.7%
28/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.1%
17/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Alanine aminotransferase increased
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
24.7%
59/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.6%
3/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
26.1%
63/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.0%
4/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Amylase increased
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.8%
9/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.9%
7/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Aspartate aminotransferase increased
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
22.6%
54/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
23.2%
56/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.5%
5/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Blood alkaline phosphatase increased
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.4%
20/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.6%
3/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.7%
21/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.5%
3/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Blood bilirubin increased
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.9%
19/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.6%
3/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.8%
14/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.0%
4/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Blood lactate dehydrogenase increased
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.5%
6/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.9%
7/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Gamma-glutamyltransferase increased
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
11.3%
27/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
4/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
10.4%
25/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Lipase increased
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
6.3%
15/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
4.6%
11/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Lymphocyte count decreased
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.1%
17/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.3%
8/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Neutrophil count decreased
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
26.4%
63/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
32.4%
78/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Platelet count decreased
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
21.8%
52/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.6%
3/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
29.0%
70/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
Weight decreased
28.6%
6/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.6%
1/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
18.4%
44/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
4/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
14.1%
34/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.5%
3/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
White blood cell count decreased
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
20.1%
48/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
26.1%
63/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Investigations
White blood cell count increased
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.3%
3/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Decreased appetite
38.1%
8/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
27.6%
66/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
4/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
26.1%
63/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.0%
4/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hyperglycaemia
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.0%
12/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.3%
20/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypoalbuminaemia
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
16.3%
39/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.6%
3/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
10.0%
24/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.0%
6/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypocalcaemia
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
12.6%
30/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.6%
3/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.4%
13/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypokalaemia
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
11.7%
28/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.6%
5/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
10.0%
24/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypomagnesaemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.0%
12/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.7%
9/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hyponatraemia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
10.9%
26/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.1%
6/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.8%
14/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Hypophosphataemia
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
14.6%
35/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.0%
2/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.5%
6/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Metabolism and nutrition disorders
Iron deficiency
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
5/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Arthralgia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
6.7%
16/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.5%
18/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Back pain
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
16.7%
3/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.5%
18/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.9%
19/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Joint swelling
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Myalgia
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.1%
17/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.1%
17/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Musculoskeletal and connective tissue disorders
Pain in extremity
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.5%
18/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
6.2%
15/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Dizziness
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
6.3%
15/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
6.6%
16/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Dysgeusia
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.4%
20/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.7%
21/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Headache
19.0%
4/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.1%
17/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.1%
17/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Neuropathy peripheral
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
13.0%
31/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
14.5%
35/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Paraesthesia
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
4.2%
10/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
4.1%
10/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Nervous system disorders
Peripheral sensory neuropathy
0.00%
0/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
9.2%
22/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
14.9%
36/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Psychiatric disorders
Delirium
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.83%
2/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Psychiatric disorders
Insomnia
14.3%
3/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.5%
18/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
10.8%
26/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Renal and urinary disorders
Dysuria
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
2.1%
5/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Renal and urinary disorders
Haematuria
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.9%
14/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
1.7%
4/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Cough
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
9.6%
23/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
10.8%
26/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Dyspnoea
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.5%
18/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.5%
18/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Respiratory, thoracic and mediastinal disorders
Epistaxis
33.3%
7/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
27.6%
66/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
8.3%
20/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Skin and subcutaneous tissue disorders
Alopecia
42.9%
9/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
34.7%
83/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
29.5%
71/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Skin and subcutaneous tissue disorders
Pruritus
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.6%
1/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
11.7%
28/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.52%
1/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
7.5%
18/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Skin and subcutaneous tissue disorders
Rash
28.6%
6/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
28.0%
67/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
18.7%
45/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Skin and subcutaneous tissue disorders
Rash maculo-papular
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.4%
13/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
3.3%
8/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Skin and subcutaneous tissue disorders
Rash papular
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.42%
1/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Hypertension
4.8%
1/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
4.6%
11/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.4%
13/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
Vascular disorders
Hypotension
9.5%
2/21 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/18 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.0%
12/239 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.00%
0/192 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
5.0%
12/241 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.
0.50%
1/200 • Adverse events were collected from the first dose through the end of the extended follow-up period (end of study), up to approximately 34 months. Deaths were recorded from study start through the end of post-treatment follow-up (end of study). On-treatment adverse events (up to 30 days after the last dose) and post-treatment follow-up events are reported separately.
All enrolled participants were included in the assessment of all-cause mortality. One safety run-in participant lost to follow-up was later confirmed (via public records) to have died \>30 days post-treatment and was only included for all-cause mortality. Serious adverse events and other adverse events were assessed only in participants who received at least one dose of the investigational product. Participants entering post-treatment follow-up (efficacy or survival) were considered at risk.

Additional Information

Study Director

Novartis Pharmaceuticals

Phone: + 1 862 778 8300

Results disclosure agreements

  • Principal investigator is a sponsor employee The terms and conditions of Novartis' agreements with its investigators may vary. However, Novartis does not prohibit any investigator from publishing. Any publications from a single-site are postponed until the publication of the pooled data (i.e., data from all sites) in the clinical trial.
  • Publication restrictions are in place

Restriction type: OTHER