Trial Outcomes & Findings for XTX202 in Patients With Advanced Solid Tumors (NCT NCT05052268)

NCT ID: NCT05052268

Last Updated: 2026-05-28

Results Overview

All participants in Phase 1 Part 1A (Dose Escalation) who received at least 1 dose of XTX202 and experienced a DLT. DLTs were defined as the following: * Any treatment-related Grade ≥ 3 toxicity * Any Grade febrile neutropenia * The following nonhematologic exceptions: * Grade 3 nausea or vomiting lasting \< 3 days * Grade 3 fatigue lasting \< 7 days * Any treatment-related toxicity that resulted in a treatment delay of ≥ 7 days

Recruitment status

COMPLETED

Study phase

PHASE1/PHASE2

Target enrollment

95 participants

Primary outcome timeframe

Cycle 1 day 1 up to just prior to the second dose of study drug at Cycle 2 day 1 (each cycle is 21 days)

Results posted on

2026-05-28

Participant Flow

In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Participant milestones

Participant milestones
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Overall Study
STARTED
1
3
3
8
13
8
13
1
2
5
1
2
15
5
15
Overall Study
COMPLETED
0
0
0
0
0
0
0
0
0
0
0
0
0
0
0
Overall Study
NOT COMPLETED
1
3
3
8
13
8
13
1
2
5
1
2
15
5
15

Reasons for withdrawal

Reasons for withdrawal
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Overall Study
Death
1
2
3
6
11
6
5
0
2
2
0
0
0
1
6
Overall Study
Investigator Decision
0
0
0
0
0
0
2
0
0
0
0
0
4
0
0
Overall Study
Lost to Follow-up
0
0
0
0
0
0
0
1
0
0
0
0
0
0
0
Overall Study
Withdrawal of Consent
0
0
0
0
1
0
1
0
0
1
0
0
1
0
0
Overall Study
Other Reason
0
1
0
2
1
2
5
0
0
2
1
2
10
4
9

Baseline Characteristics

XTX202 in Patients With Advanced Solid Tumors

Baseline characteristics by cohort

Baseline characteristics by cohort
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
n=1 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=15 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=5 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=15 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Total
n=95 Participants
Total of all reporting groups
Age, Continuous
67 years
STANDARD_DEVIATION 0 • n=51 Participants
69.7 years
STANDARD_DEVIATION 16.2 • n=14 Participants
61.7 years
STANDARD_DEVIATION 14.64 • n=65 Participants
65.1 years
STANDARD_DEVIATION 10.80 • n=24 Participants
62.5 years
STANDARD_DEVIATION 13.29 • n=107 Participants
64.1 years
STANDARD_DEVIATION 12.59 • n=1000 Participants
68.0 years
STANDARD_DEVIATION 8.40
64 years
STANDARD_DEVIATION 0 • n=204 Participants
37 years
STANDARD_DEVIATION 16.97
68.8 years
STANDARD_DEVIATION 6.06 • n=792 Participants
62 years
STANDARD_DEVIATION 0 • n=20 Participants
58.0 years
STANDARD_DEVIATION 15.56 • n=20 Participants
63.3 years
STANDARD_DEVIATION 11.01 • n=260 Participants
58.8 years
STANDARD_DEVIATION 17.05 • n=5 Participants
62.7 years
STANDARD_DEVIATION 11.32 • n=4 Participants
63.5 years
STANDARD_DEVIATION 11.91 • n=4 Participants
Age, Customized
<65
0 Participants
n=51 Participants
1 Participants
n=14 Participants
2 Participants
n=65 Participants
4 Participants
n=24 Participants
6 Participants
n=107 Participants
3 Participants
n=1000 Participants
4 Participants
1 Participants
n=204 Participants
2 Participants
1 Participants
n=792 Participants
1 Participants
n=20 Participants
1 Participants
n=20 Participants
7 Participants
n=260 Participants
3 Participants
n=5 Participants
9 Participants
n=4 Participants
45 Participants
n=4 Participants
Age, Customized
≥ 60 to <75
1 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
3 Participants
n=24 Participants
5 Participants
n=107 Participants
4 Participants
n=1000 Participants
7 Participants
0 Participants
n=204 Participants
0 Participants
3 Participants
n=792 Participants
0 Participants
n=20 Participants
1 Participants
n=20 Participants
5 Participants
n=260 Participants
2 Participants
n=5 Participants
4 Participants
n=4 Participants
35 Participants
n=4 Participants
Age, Customized
≥ 75
0 Participants
n=51 Participants
2 Participants
n=14 Participants
1 Participants
n=65 Participants
1 Participants
n=24 Participants
2 Participants
n=107 Participants
1 Participants
n=1000 Participants
2 Participants
0 Participants
n=204 Participants
0 Participants
1 Participants
n=792 Participants
0 Participants
n=20 Participants
0 Participants
n=20 Participants
3 Participants
n=260 Participants
0 Participants
n=5 Participants
2 Participants
n=4 Participants
15 Participants
n=4 Participants
Sex: Female, Male
Female
0 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
4 Participants
n=24 Participants
6 Participants
n=107 Participants
4 Participants
n=1000 Participants
4 Participants
0 Participants
n=204 Participants
1 Participants
3 Participants
n=792 Participants
0 Participants
n=20 Participants
0 Participants
n=20 Participants
8 Participants
n=260 Participants
2 Participants
n=5 Participants
7 Participants
n=4 Participants
39 Participants
n=4 Participants
Sex: Female, Male
Male
1 Participants
n=51 Participants
3 Participants
n=14 Participants
3 Participants
n=65 Participants
4 Participants
n=24 Participants
7 Participants
n=107 Participants
4 Participants
n=1000 Participants
9 Participants
1 Participants
n=204 Participants
1 Participants
2 Participants
n=792 Participants
1 Participants
n=20 Participants
2 Participants
n=20 Participants
7 Participants
n=260 Participants
3 Participants
n=5 Participants
8 Participants
n=4 Participants
56 Participants
n=4 Participants
Ethnicity (NIH/OMB)
Hispanic or Latino
0 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
1 Participants
n=24 Participants
0 Participants
n=107 Participants
1 Participants
n=1000 Participants
1 Participants
0 Participants
n=204 Participants
0 Participants
0 Participants
n=792 Participants
0 Participants
n=20 Participants
1 Participants
n=20 Participants
4 Participants
n=260 Participants
1 Participants
n=5 Participants
2 Participants
n=4 Participants
11 Participants
n=4 Participants
Ethnicity (NIH/OMB)
Not Hispanic or Latino
1 Participants
n=51 Participants
3 Participants
n=14 Participants
3 Participants
n=65 Participants
7 Participants
n=24 Participants
13 Participants
n=107 Participants
7 Participants
n=1000 Participants
12 Participants
1 Participants
n=204 Participants
2 Participants
4 Participants
n=792 Participants
1 Participants
n=20 Participants
1 Participants
n=20 Participants
10 Participants
n=260 Participants
4 Participants
n=5 Participants
12 Participants
n=4 Participants
81 Participants
n=4 Participants
Ethnicity (NIH/OMB)
Unknown or Not Reported
0 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
0 Participants
n=24 Participants
0 Participants
n=107 Participants
0 Participants
n=1000 Participants
0 Participants
0 Participants
n=204 Participants
0 Participants
1 Participants
n=792 Participants
0 Participants
n=20 Participants
0 Participants
n=20 Participants
1 Participants
n=260 Participants
0 Participants
n=5 Participants
1 Participants
n=4 Participants
3 Participants
n=4 Participants
Race/Ethnicity, Customized
American Indian or Alaska Native
0 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
0 Participants
n=24 Participants
0 Participants
n=107 Participants
0 Participants
n=1000 Participants
0 Participants
0 Participants
n=204 Participants
0 Participants
0 Participants
n=792 Participants
0 Participants
n=20 Participants
0 Participants
n=20 Participants
0 Participants
n=260 Participants
0 Participants
n=5 Participants
0 Participants
n=4 Participants
0 Participants
n=4 Participants
Race/Ethnicity, Customized
Asian
0 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
0 Participants
n=24 Participants
3 Participants
n=107 Participants
1 Participants
n=1000 Participants
0 Participants
0 Participants
n=204 Participants
0 Participants
0 Participants
n=792 Participants
0 Participants
n=20 Participants
0 Participants
n=20 Participants
0 Participants
n=260 Participants
0 Participants
n=5 Participants
0 Participants
n=4 Participants
4 Participants
n=4 Participants
Race/Ethnicity, Customized
Black or African American
0 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
1 Participants
n=24 Participants
1 Participants
n=107 Participants
0 Participants
n=1000 Participants
1 Participants
0 Participants
n=204 Participants
0 Participants
1 Participants
n=792 Participants
0 Participants
n=20 Participants
0 Participants
n=20 Participants
3 Participants
n=260 Participants
0 Participants
n=5 Participants
1 Participants
n=4 Participants
8 Participants
n=4 Participants
Race/Ethnicity, Customized
Native Hawaiian or other Pacific Islander
0 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
0 Participants
n=24 Participants
0 Participants
n=107 Participants
0 Participants
n=1000 Participants
0 Participants
0 Participants
n=204 Participants
0 Participants
0 Participants
n=792 Participants
0 Participants
n=20 Participants
0 Participants
n=20 Participants
0 Participants
n=260 Participants
0 Participants
n=5 Participants
0 Participants
n=4 Participants
0 Participants
n=4 Participants
Race/Ethnicity, Customized
White
1 Participants
n=51 Participants
3 Participants
n=14 Participants
3 Participants
n=65 Participants
7 Participants
n=24 Participants
9 Participants
n=107 Participants
7 Participants
n=1000 Participants
11 Participants
1 Participants
n=204 Participants
2 Participants
4 Participants
n=792 Participants
1 Participants
n=20 Participants
2 Participants
n=20 Participants
12 Participants
n=260 Participants
4 Participants
n=5 Participants
14 Participants
n=4 Participants
81 Participants
n=4 Participants
Race/Ethnicity, Customized
Other
0 Participants
n=51 Participants
0 Participants
n=14 Participants
0 Participants
n=65 Participants
0 Participants
n=24 Participants
0 Participants
n=107 Participants
0 Participants
n=1000 Participants
1 Participants
0 Participants
n=204 Participants
0 Participants
0 Participants
n=792 Participants
0 Participants
n=20 Participants
0 Participants
n=20 Participants
0 Participants
n=260 Participants
1 Participants
n=5 Participants
0 Participants
n=4 Participants
2 Participants
n=4 Participants

PRIMARY outcome

Timeframe: Cycle 1 day 1 up to just prior to the second dose of study drug at Cycle 2 day 1 (each cycle is 21 days)

All participants in Phase 1 Part 1A (Dose Escalation) who received at least 1 dose of XTX202 and experienced a DLT. DLTs were defined as the following: * Any treatment-related Grade ≥ 3 toxicity * Any Grade febrile neutropenia * The following nonhematologic exceptions: * Grade 3 nausea or vomiting lasting \< 3 days * Grade 3 fatigue lasting \< 7 days * Any treatment-related toxicity that resulted in a treatment delay of ≥ 7 days

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Dose Limiting Toxicities (DLTs) (Phase 1 Part 1A Only)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants

PRIMARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 1 Part 1A and Part 1B.

Treatment-emergent adverse event (TEAE) is defined as any adverse event that starts or increases in severity on or after the first dose of study drug and no later than 90 days after the last dose of study drug. Adverse events are graded using the NCI CTCAE version 5.0.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
n=1 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Treatment-emergent Adverse Events (Phase 1 Only)
13 Number of participants with TEAE
8 Number of participants with TEAE
13 Number of participants with TEAE
1 Number of participants with TEAE
2 Number of participants with TEAE
5 Number of participants with TEAE
1 Number of participants with TEAE
1 Number of participants with TEAE
2 Number of participants with TEAE
3 Number of participants with TEAE
8 Number of participants with TEAE

PRIMARY outcome

Timeframe: Up to 24 months

Population: All participants in Phase 2 Part 2A and Part 2B with measurable disease at baseline who received XTX202 and had at least 1 post-Baseline response assessment or discontinued treatment due to disease progression (including death caused by disease progression) prior to the first efficacy evaluation were included in the analysis set.

Percentage of participants who achieved at least one confirmed Complete Response (CR) or Partial Response (PR). Response is based on Investigator assessment according to RECIST v1.1. In the analysis set used for ORR, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=14 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=6 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=13 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Investigator-assessed Objective Response Rate (ORR) Per RECIST 1.1 (Phase 2 Only)
0 Percentage of participants
Interval 0.0 to 84.2
0 Percentage of participants
Interval 0.0 to 23.2
16.7 Percentage of participants
Interval 0.4 to 64.1
0 Percentage of participants
Interval 0.0 to 24.7

PRIMARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 1 Part 1A and Part 1B with both baseline and at least one post-baseline result.

Number of participants that experienced a clinical laboratory test abnormality. Abnormalities considered are those Grade 3-4 events with a \>= 1 grade increase from baseline. Baseline is defined as the last available measurement taken prior to the first administration of study treatment. Laboratory data is graded using the NCI CTCAE version 5.0. Participants are included only once, in the highest level of CTCAE Grade.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
n=1 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Alanine Aminotransferase increased - Grade 3
0 Participants
0 Participants
2 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Alanine Aminotransferase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Albumin decreased (Hypoalbuminemia) - Grade 3
1 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Albumin decreased (Hypoalbuminemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Alkaline Phosphatase increased - Grade 3
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Alkaline Phosphatase increased - Garde 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Aspartate Aminotransferase increased - Grade 3
0 Participants
2 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Aspartate Aminotransferase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Blood Bilirubin increased - Grade 3
0 Participants
1 Participants
2 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Blood Bilirubin increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Calcium decreased (Hypocalcemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Calcium decreased (Hypocalcemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Calcium increased (Hypercalcemia) - Grade 3
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Calcium increased (Hypercalcemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Creatinine increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Creatinine increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Glucose decreased (Hypoglycemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Glucose decreased (Hypoglycemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Lipase increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Lipase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Magnesium decreased (Hypomagnesemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Magnesium decreased (Hypomagnesemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Magnesium increased (Hypermagnesemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Magnesium increased (Hypermagnesemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Potassium decreased (Hypokalemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Potassium decreased (Hypokalemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Potassium increased (Hyperkalemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Potassium increased (Hyperkalemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Serum Amylase increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Serum Amylase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Sodium decreased (Hyponatremia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Sodium decreased (Hyponatremia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Sodium increased (Hypernatremia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Biochemistry
Sodium increased (Hypernatremia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants

PRIMARY outcome

Timeframe: up to 24 months

Population: All participants who received XTX202 in Phase 1 Part 1A and Part 1B with both baseline and at least one post-baseline result.

Number of participants that experienced a clinical laboratory test abnormality. Abnormalities considered are those Grade 3-4 events with a \>= 1 grade increase from baseline. Baseline is defined as the last available measurement taken prior to the first administration of study treatment. Laboratory data is graded using the NCI CTCAE version 5.0. Participants are included only once, in the highest level of CTCAE Grade.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
n=1 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Hemoglobin increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Lymphocyte count decreased - Grade 3
5 Participants
4 Participants
6 Participants
1 Participants
1 Participants
0 Participants
1 Participants
0 Participants
2 Participants
0 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Lymphocyte count decreased - Grade 4
0 Participants
1 Participants
2 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Lymphocyte count increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Anemia (Hemoglobin decreased) - Grade 3
3 Participants
1 Participants
4 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Anemia (Hemoglobin decreased) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Hemoglobin increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Neutrophil count decreased - Grade 3
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Lymphocyte count increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Neutrophil count decreased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
White Blood Cells decreased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Platelets count decreased - Grade 3
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
Platelets count decreased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Hematology
White Blood Cells decreased - Grade 3
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants

PRIMARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 1 Part 1A and Part 1B with both baseline and at least one post-baseline result.

Number of participants with shift from baseline in laboratory results. Baseline is defined as the last available measurement taken prior to the first administration of study treatment. Participants with both baseline and at least one postbaseline result are included. Participants are included only once, in the highest level of CTCAE Grade. Missing = number of patients with missing baseline and/or post baseline laboratory value.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
n=1 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · Missing
1 Participants
3 Participants
3 Participants
0 Participants
1 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · Low (at baseline) to Normal (at post baseline)
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
2 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · Normal (at baseline) to Normal (at post baseline)
4 Participants
4 Participants
4 Participants
0 Participants
1 Participants
2 Participants
0 Participants
1 Participants
3 Participants
0 Participants
3 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · Normal (at baseline) to High (at post baseline)
3 Participants
1 Participants
2 Participants
0 Participants
0 Participants
1 Participants
1 Participants
0 Participants
0 Participants
2 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyrotropin (mIU/L) · High (at baseline) to High (at post baseline)
4 Participants
0 Participants
1 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Low (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Normal (at baseline) to Low (at post baseline)
0 Participants
1 Participants
2 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Normal (at baseline) to Normal (at post baseline)
12 Participants
4 Participants
7 Participants
1 Participants
1 Participants
3 Participants
1 Participants
1 Participants
3 Participants
3 Participants
5 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Normal (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · High (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Missing
1 Participants
3 Participants
4 Participants
0 Participants
1 Participants
2 Participants
0 Participants
0 Participants
0 Participants
0 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Low (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Normal (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Normal (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · High (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Missing
13 Participants
8 Participants
12 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
2 Participants
3 Participants
8 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Low (at baseline) to Low (at post baseline)
9 Participants
1 Participants
3 Participants
1 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
2 Participants
3 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Low (at baseline) to Normal (at post baseline)
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Normal (at baseline) to Low (at post baseline)
0 Participants
1 Participants
1 Participants
0 Participants
0 Participants
1 Participants
0 Participants
1 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Normal (at baseline) to Normal (at post baseline)
2 Participants
2 Participants
4 Participants
0 Participants
0 Participants
2 Participants
1 Participants
0 Participants
1 Participants
0 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Normal (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · High (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Missing
1 Participants
4 Participants
5 Participants
0 Participants
1 Participants
1 Participants
0 Participants
0 Participants
1 Participants
0 Participants
2 Participants

PRIMARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 1 Part 1A and Part 1B with both baseline and at least one post-baseline result.

Number of participants with shift from baseline in laboratory results. Baseline is defined as the last available measurement taken prior to the first administration of study treatment. Participants with both baseline and at least one postbaseline result are included. Participants are included only once, in the highest level of CTCAE Grade. Missing = number of patients with missing baseline and/or post baseline laboratory value. Missing = number of patients with missing baseline and/or post baseline laboratory value

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
n=1 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · Normal (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · Normal (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · High (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · Missing
5 Participants
5 Participants
9 Participants
0 Participants
0 Participants
1 Participants
0 Participants
1 Participants
1 Participants
0 Participants
3 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Low (at baseline) to Normal (at post baseline)
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · High (at baseline) to High (at post baseline)
3 Participants
0 Participants
3 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Low (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Normal (at baseline) to Normal (at post baseline)
2 Participants
3 Participants
5 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
1 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Normal (at baseline) to High (at post baseline)
1 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · High (at baseline) to High (at post baseline)
4 Participants
1 Participants
2 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Missing
6 Participants
4 Participants
4 Participants
1 Participants
2 Participants
5 Participants
1 Participants
0 Participants
2 Participants
1 Participants
3 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · Low (at baseline) to Low (at post baseline)
8 Participants
3 Participants
4 Participants
1 Participants
2 Participants
4 Participants
1 Participants
0 Participants
2 Participants
3 Participants
5 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · Low (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Partial Thromboplastin Time (sec) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Normal (at baseline) to Normal (at post baseline)
9 Participants
3 Participants
8 Participants
0 Participants
1 Participants
3 Participants
1 Participants
1 Participants
2 Participants
3 Participants
6 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Normal (at baseline) to High (at post baseline)
1 Participants
3 Participants
2 Participants
0 Participants
1 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Missing
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · Low (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · Normal (at baseline) to Normal (at post baseline)
5 Participants
4 Participants
7 Participants
1 Participants
1 Participants
2 Participants
0 Participants
1 Participants
1 Participants
1 Participants
3 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · Normal (at baseline) to High (at post baseline)
4 Participants
3 Participants
2 Participants
0 Participants
0 Participants
2 Participants
1 Participants
0 Participants
0 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · High (at baseline) to High (at post baseline)
4 Participants
0 Participants
3 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
1 Participants
1 Participants
5 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 1 Only) - Coagulation
Prothrombin Time (sec) · Missing
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
0 Participants
0 Participants
0 Participants

SECONDARY outcome

Timeframe: Up to 24 months

Population: All subjects in Phase 1 Part 1A and Part 1B with measurable disease at baseline who received XTX202 and had at least 1 post-Baseline response assessment or discontinued treatment due to disease progression (including death caused by disease progression) prior to the first efficacy evaluation.

Percentage of participants who achieved at least one confirmed Complete Response (CR) or Partial Response (PR). Response will be based on Investigator's assessment according to RECIST v1.1.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=11 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=4 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Investigator-assessed Objective Response Rate (ORR) Per RECIST 1.1 (Phase 1 Only)
0 Percentage of participants
Interval 0.0 to 28.5
0 Percentage of participants
Interval 0.0 to 41.0
0 Percentage of participants
Interval 0.0 to 28.5
0 Percentage of participants
Interval 0.0 to 97.5
0 Percentage of participants
Interval 0.0 to 84.2
0 Percentage of participants
Interval 0.0 to 45.9
0 Percentage of participants
Interval 0.0 to 97.5
0 Percentage of participants
Interval 0.0 to 70.8
0 Percentage of participants
Interval 0.0 to 60.2
0 Percentage of participants
Interval 0.0 to 36.9

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants in Phase 2 Part 2A and Part 2B with measurable disease at baseline who received XTX202 and had at least 1 post-Baseline response assessment or discontinued treatment due to disease progression (including death caused by disease progression) prior to the first efficacy evaluation and had a confirmed objective response (CR or PR).

Duration of response is defined as time from first documentation of a subsequently confirmed objective response (CR or PR) to the date of the first documentation of radiographic disease progression according to Investigator assessment by RECIST v1.1, or death due to any cause, whichever occurs first. Participants who do not have an observed documented disease progression or death from any cause will be censored at the latest tumor response assessment date.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=1 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Duration of Response (DOR) (Phase 2 Only)
NA Days
Median DOR and 95% confidence interval could not be determined because the single participant with PR remained in PR until the End-of-Treatment visit scan

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants in Phase 2 Part 2A and Part 2B with measurable disease at baseline who received XTX202 and had at least 1 post-Baseline response assessment or discontinued treatment due to disease progression (including death caused by disease progression) prior to the first efficacy evaluation were included in the analysis set.

Disease Control Rate (DCR) is defined as percentage of participants with confirmed BOR of CR, PR or SD (minimum duration of 6 weeks) according to RECIST v1.1, after the first dose of study treatment. In the analysis set used for DCR, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=14 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=6 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=13 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Disease Control Rate (Phase 2 Only)
100 Percentage of participants
Interval 15.8 to 100.0
50 Percentage of participants
Interval 23.0 to 77.0
50 Percentage of participants
Interval 11.8 to 88.2
53.8 Percentage of participants
Interval 25.1 to 80.8

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 2 Part 2A and Part 2B were included in the analysis set

OS is defined as the time from first administration of study treatment to death due to any cause. For participants without a record of death, OS will be censored at the date they were last known alive. In the analysis set used for OS, participants are assigned to a treatment group based on the initial dose received.. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=15 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=6 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=14 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Overall Survival (OS) (Phase 2 Only)
NA months
Median OS was not reached. 95% Confidence Interval not evaluable due to insufficient number of participants with events.
NA months
Median OS was not reached. 95% Confidence Interval not evaluable due to insufficient number of participants with events.
NA months
Interval 6.1 to
Median OS was not reached. Upper limit of 95% Confidence Interval not evaluable due to insufficient number of participants with events.
NA months
Interval 3.9 to
Median OS was not reached. Upper limit of 95% Confidence Interval not evaluable due to insufficient number of participants with events.

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 2 Part 2A and Part 2B were included in the analysis set.

PFS is defined as the time from first administration of study treatment until first documentation of radiographic PD according to RECIST v1.1, or death due to any cause, whichever occurs first. Participants who do not have an observed documented disease progression or death from any cause will be censored at the latest tumor response assessment date. In the analysis set used for PFS, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=15 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=6 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=14 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Progression-free Survival (PFS) (Phase 2 Only)
4.1 months
Interval 4.0 to
"Upper Limit 95% Confidence Interval not evaluable due to insufficient number of participants with events"
4.1 months
Interval 2.0 to 8.4
3.1 months
Interval 2.1 to
"Upper Limit 95% Confidence Interval not evaluable due to insufficient number of participants with events"
2.7 months
Interval 1.0 to 4.1

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 2 Part 2A and Part 2B.

Treatment-emergent adverse event is defined as any adverse event (AE) that starts or increases in severity on or after the first dose of study drug and no later than 90 days after the last dose of study drug. AEs are graded using the NCI CTCAE version 5.0.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=15 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=5 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=15 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Treatment-emergent Adverse Events (Phase 2 Only)
2 Number of participants with TEAE
15 Number of participants with TEAE
5 Number of participants with TEAE
15 Number of participants with TEAE

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 2 Part 2A and Part 2B with both baseline and at least one post-baseline result.

Number of participants that experienced a clinical laboratory test abnormality. Abnormalities considered are those Grade 3-4 events with a \>= 1 grade increase from baseline. Baseline is defined as the last available measurement taken prior to the first administration of study treatment. Laboratory data is graded using the NCI CTCAE version 5.0. Participants are included only once, in the highest level of CTCAE Grade.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=15 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=5 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=15 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Anemia (Hemoglobin decreased) - Grade 3
0 Participants
1 Participants
1 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Anemia (Hemoglobin decreased) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Hemoglobin increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Hemoglobin increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Lymphocyte count decreased - Grade 3
1 Participants
7 Participants
1 Participants
7 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Lymphocyte count decreased - Grade 4
0 Participants
0 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Lymphocyte count increased - Grade 3
0 Participants
2 Participants
0 Participants
3 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Lymphocyte count increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Neutrophil count decreased - Grade 3
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Neutrophil count decreased - Grade 4
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Platelets count decreased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
Platelets count decreased - Grade 4
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
White Blood Cells decreased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Hematology
White Blood Cells decreased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 2 Part 2A and Part 2B with both baseline and at least one post-baseline result.

Number of participants that experienced a clinical laboratory test abnormality. Abnormalities considered are those Grade 3-4 events with a \>= 1 grade increase from baseline. Baseline is defined as the last available measurement taken prior to the first administration of study treatment. Laboratory data is graded using the NCI CTCAE version 5.0. Participants are included only once, in the highest level of CTCAE Grade.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=15 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=5 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=15 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Alanine Aminotransferase increased - Grade 3
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Alanine Aminotransferase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Albumin decreased (Hypoalbuminemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Albumin decreased (Hypoalbuminemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Alkaline Phosphatase increased - Grade 3
0 Participants
0 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Alkaline Phosphatase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Aspartate Aminotransferase increased - Grade 3
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Aspartate Aminotransferase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Blood Bilirubin increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Blood Bilirubin increased- Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Calcium decreased (Hypocalcemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Calcium decreased (Hypocalcemia) - Grade 4
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Calcium increased (Hypercalcemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Calcium increased (Hypercalcemia) - Grade 4
0 Participants
2 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Creatinine increased - Grade 3
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Creatinine increased - Grade 4
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Glucose decreased (Hypoglycemia) - Grade 3
0 Participants
0 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Glucose decreased (Hypoglycemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Lipase increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Lipase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Magnesium decreased (Hypomagnesemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Magnesium decreased (Hypomagnesemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Magnesium increased (Hypermagnesemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Magnesium increased (Hypermagnesemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Potassium decreased (Hypokalemia) - Grade 3
0 Participants
0 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Potassium decreased (Hypokalemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Potassium increased (Hyperkalemia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Potassium increased (Hyperkalemia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Serum Amylase increased - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Serum Amylase increased - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Sodium decreased (Hyponatremia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Sodium decreased (Hyponatremia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Sodium increased (Hypernatremia) - Grade 3
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Biochemistry
Sodium increased (Hypernatremia) - Grade 4
0 Participants
0 Participants
0 Participants
0 Participants

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 2 Part 2A and Part 2B with both baseline and at least one post-baseline result.

Number of participants with shift from baseline in laboratory results. Baseline is defined as the last available measurement taken prior to the first administration of study treatment. Participants with both baseline and at least one postbaseline result are included. Participants are included only once, in the highest level of CTCAE Grade. Missing = number of patients with missing baseline and/or post baseline laboratory value.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=15 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=5 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=15 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · Low (at baseline) to Normal (at post baseline)
1 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · Low (at baseline) to High (at post baseline)
0 Participants
1 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · Normal (at baseline) to Normal (at post baseline)
0 Participants
4 Participants
2 Participants
7 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · Normal (at baseline) to High (at post baseline)
0 Participants
4 Participants
1 Participants
3 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · High (at baseline) to Normal (at post baseline)
1 Participants
2 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · High (at baseline) to High (at post baseline)
0 Participants
2 Participants
0 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyrotropin (mIU/L) · Missing
0 Participants
2 Participants
0 Participants
3 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Low (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
1 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Normal (at baseline) to Normal (at post baseline)
2 Participants
13 Participants
4 Participants
10 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Normal (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · High (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Thyroxine, Free (pmol/L) · Missing
0 Participants
2 Participants
0 Participants
4 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Low (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Low (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Normal (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Normal (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Normal (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · High (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine (nmol/L) · Missing
2 Participants
15 Participants
5 Participants
15 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Low (at baseline) to Low (at post baseline)
1 Participants
5 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Low (at baseline) to Normal (at post baseline)
0 Participants
1 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Low (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Normal (at baseline) to Low (at post baseline)
0 Participants
3 Participants
2 Participants
6 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Normal (at baseline) to Normal (at post baseline)
1 Participants
2 Participants
3 Participants
4 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Normal (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · High (at baseline) to Low (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · High (at baseline) to Normal (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · High (at baseline) to High (at post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Thyroid Function
Triiodothyronine, Free (pmol/L) · Missing
0 Participants
4 Participants
0 Participants
4 Participants

SECONDARY outcome

Timeframe: Up to 24 months

Population: All participants who received XTX202 in Phase 2 Part 2A and Part 2B with both baseline and at least one post-baseline result.

Number of participants with shift from baseline in laboratory results. Baseline is defined as the last available measurement taken prior to the first administration of study treatment. Participants with both baseline and at least one postbaseline result are included. Participants are included only once, in the highest level of CTCAE Grade. Missing = number of patients with missing baseline and/or post baseline laboratory value.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=15 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=5 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=15 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · High (at baseline) to High (post baseline)
0 Participants
3 Participants
1 Participants
4 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Low (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Low (at baseline) to Normal (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Low (at baseline) to High (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Normal (at baseline) to Low (post baseline)
0 Participants
1 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Normal (at baseline) to Normal (post baseline)
0 Participants
4 Participants
2 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Normal (at baseline) to High (post baseline)
1 Participants
1 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · High (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · High (at baseline) to Normal (post baseline)
1 Participants
2 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · High (at baseline) to High (post baseline)
0 Participants
3 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Activated Partial Thromboplastin Time (sec) · Missing
0 Participants
4 Participants
3 Participants
13 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · Low (at baseline) to Low (post baseline)
0 Participants
4 Participants
3 Participants
13 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · Low (at baseline) to Normal (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · Low (at baseline) to High (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · Normal (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · Normal (at baseline) to Normal (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · Normal (at baseline) to High (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · High (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · High (at baseline) to Normal (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · High (at baseline) to High (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Partial Thromboplastin Time (sec) · Missing
2 Participants
11 Participants
2 Participants
2 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Low (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Low (at baseline) to Normal (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Low (at baseline) to High (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Normal (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Normal (at baseline) to Normal (post baseline)
2 Participants
11 Participants
4 Participants
12 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Normal (at baseline) to High (post baseline)
0 Participants
2 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · High (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · High (at baseline) to Normal (post baseline)
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · High (at baseline) to High (post baseline)
0 Participants
2 Participants
1 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Intl. Normalized Ratio · Missing
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · Low (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · Low (at baseline) to Normal (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · Low (at baseline) to High (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · Normal (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · Normal (at baseline) to Normal (post baseline)
1 Participants
9 Participants
2 Participants
5 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · Normal (at baseline) to High (post baseline)
1 Participants
3 Participants
2 Participants
5 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · High (at baseline) to Low (post baseline)
0 Participants
0 Participants
0 Participants
0 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · High (at baseline) to Normal (post baseline)
0 Participants
0 Participants
0 Participants
1 Participants
Incidence of Changes in Clinical Laboratory Values (Phase 2 Only) - Coagulation
Prothrombin Time (sec) · Missing
0 Participants
0 Participants
0 Participants
0 Participants

SECONDARY outcome

Timeframe: 0.00, 0.0167, 0.250, 0.500, 1.50, 3.00, 24.0, 72.0, 144, 312, 504 hours post-dose following a single administration of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Plasma Concentration of Total XTX202 by Nominal Time (h) From End of Infusion Following a Single IV Administration of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=5 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=7 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Plasma Concentrations of Total XTX202
3.00 hours
20200 ng/mL
Standard Deviation 4940
32600 ng/mL
Standard Deviation 9800
55500 ng/mL
Standard Deviation 11000
13900 ng/mL
22900 ng/mL
Standard Deviation 9900
39500 ng/mL
Standard Deviation 10600
22700 ng/mL
Standard Deviation 1200
49500 ng/mL
Standard Deviation 9930
18100 ng/mL
Standard Deviation 7220
63900 ng/mL
Standard Deviation 14500
3580 ng/mL
Standard Deviation 0
4710 ng/mL
Standard Deviation 1110
5840 ng/mL
Standard Deviation 715
12400 ng/mL
Standard Deviation 3960
Plasma Concentrations of Total XTX202
0.00 hours
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
NA ng/mL
Below the level of detection
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
NA ng/mL
Standard Deviation 0
Below the level of detection
NA ng/mL
Standard Deviation 0
Below the level of detection
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
Plasma Concentrations of Total XTX202
0.0167 hours
25400 ng/mL
Standard Deviation 7120
46900 ng/mL
Standard Deviation 12500
60800 ng/mL
Standard Deviation 27600
NA ng/mL
Sample collected at incorrect time
NA ng/mL
Standard Deviation NA
Not calculated
48900 ng/mL
Standard Deviation 13600
26600 ng/mL
Standard Deviation 2830
75500 ng/mL
Standard Deviation 11400
25800 ng/mL
Standard Deviation 5690
87700 ng/mL
Standard Deviation 13400
NA ng/mL
Sample collected at incorrect time
6400 ng/mL
Standard Deviation 0
7320 ng/mL
Standard Deviation 912
20400 ng/mL
Standard Deviation 5590
Plasma Concentrations of Total XTX202
0.250 hours
23500 ng/mL
Standard Deviation 5260
49700 ng/mL
Standard Deviation 14600
77800 ng/mL
Standard Deviation 15100
NA ng/mL
Sample collected at incorrect time
38000 ng/mL
Standard Deviation NA
Not calculated
49900 ng/mL
Standard Deviation 12400
28600 ng/mL
Standard Deviation 6430
80400 ng/mL
Standard Deviation 8280
27900 ng/mL
Standard Deviation 5060
78600 ng/mL
Standard Deviation 14300
NA ng/mL
Standard Deviation 0
Below the level of detection
8420 ng/mL
Standard Deviation 0
6700 ng/mL
Standard Deviation 1230
15900 ng/mL
Standard Deviation 4990
Plasma Concentrations of Total XTX202
0.500 hours
23700 ng/mL
Standard Deviation 7540
46200 ng/mL
Standard Deviation 14300
74200 ng/mL
Standard Deviation 15800
NA ng/mL
Sample collected at incorrect time
34600 ng/mL
Standard Deviation NA
Not calculated
47500 ng/mL
Standard Deviation 13500
28000 ng/mL
Standard Deviation 5090
72800 ng/mL
Standard Deviation 10400
27400 ng/mL
Standard Deviation 5310
78000 ng/mL
Standard Deviation 18200
4170 ng/mL
Standard Deviation 0
7300 ng/mL
Standard Deviation 2270
6260 ng/mL
Standard Deviation 1130
15400 ng/mL
Standard Deviation 5480
Plasma Concentrations of Total XTX202
1.50 hours
21500 ng/mL
Standard Deviation 5150
39900 ng/mL
Standard Deviation 14000
68000 ng/mL
Standard Deviation 12300
15900 ng/mL
27300 ng/mL
Standard Deviation 8700
41800 ng/mL
Standard Deviation 9930
23000 ng/mL
Standard Deviation 3110
64800 ng/mL
Standard Deviation 12400
26100 ng/mL
Standard Deviation 6270
65300 ng/mL
Standard Deviation 13800
4410 ng/mL
Standard Deviation 0
4970 ng/mL
Standard Deviation 1880
5940 ng/mL
Standard Deviation 735
13400 ng/mL
Standard Deviation 4170
Plasma Concentrations of Total XTX202
24.0 hours
12700 ng/mL
Standard Deviation 3010
20900 ng/mL
Standard Deviation 6720
32500 ng/mL
Standard Deviation 8180
8070 ng/mL
13400 ng/mL
Standard Deviation 3610
30200 ng/mL
Standard Deviation NA
Not calculated
14900 ng/mL
Standard Deviation NA
Not calculated
27100 ng/mL
Standard Deviation NA
Not calculated
15000 ng/mL
Standard Deviation 5370
2580 ng/mL
Standard Deviation 0
3500 ng/mL
Standard Deviation 575
4220 ng/mL
Standard Deviation 1040
7470 ng/mL
Standard Deviation 1940
Plasma Concentrations of Total XTX202
72.0 hours
7210 ng/mL
Standard Deviation 1270
11800 ng/mL
Standard Deviation 5180
17900 ng/mL
Standard Deviation 5850
NA ng/mL
Sample collected at incorrect time
8280 ng/mL
Standard Deviation 2410
14500 ng/mL
Standard Deviation 4550
7960 ng/mL
Standard Deviation 2110
15100 ng/mL
Standard Deviation 2870
8850 ng/mL
Standard Deviation 3340
18600 ng/mL
Standard Deviation 4200
1410 ng/mL
Standard Deviation 0
1740 ng/mL
Standard Deviation 21.2
2150 ng/mL
Standard Deviation 7.07
4380 ng/mL
Standard Deviation 1950
Plasma Concentrations of Total XTX202
144 hours
4920 ng/mL
Standard Deviation 1040
7180 ng/mL
Standard Deviation 3380
10500 ng/mL
Standard Deviation 3030
3180 ng/mL
7060 ng/mL
Standard Deviation NA
Not calculated
8250 ng/mL
Standard Deviation 2690
5850 ng/mL
Standard Deviation 1090
11500 ng/mL
Standard Deviation 3650
5230 ng/mL
Standard Deviation 1560
9360 ng/mL
Standard Deviation 1580
955 ng/mL
Standard Deviation 0
1240 ng/mL
Standard Deviation 401
1540 ng/mL
Standard Deviation 400
2880 ng/mL
Standard Deviation 951
Plasma Concentrations of Total XTX202
312 hours
2460 ng/mL
Standard Deviation 815
4500 ng/mL
Standard Deviation 2120
6120 ng/mL
Standard Deviation 1800
1550 ng/mL
2230 ng/mL
Standard Deviation NA
Not calculated
5390 ng/mL
Standard Deviation 2090
3080 ng/mL
Standard Deviation 841
5560 ng/mL
Standard Deviation 1100
3260 ng/mL
Standard Deviation 1380
5350 ng/mL
Standard Deviation 1530
628 ng/mL
Standard Deviation 0
770 ng/mL
Standard Deviation 385
1090 ng/mL
Standard Deviation 264
1990 ng/mL
Standard Deviation 663
Plasma Concentrations of Total XTX202
504 hours
1500 ng/mL
Standard Deviation 336
1990 ng/mL
Standard Deviation 893
3910 ng/mL
Standard Deviation 1340
1180 ng/mL
1480 ng/mL
Standard Deviation NA
Not calculated
3160 ng/mL
Standard Deviation 1290
1810 ng/mL
Standard Deviation 424
3090 ng/mL
Standard Deviation 233
1950 ng/mL
Standard Deviation 1400
3030 ng/mL
Standard Deviation 1360
363 ng/mL
Standard Deviation 0
433 ng/mL
Standard Deviation 225
3600 ng/mL
Standard Deviation 5360
992 ng/mL
Standard Deviation 414

SECONDARY outcome

Timeframe: 0.00, 0.0167, 0.250, 0.500, 1.50, 3.00, 24.0, 72.0, 144, 312, 504 hours post-dose following a single administration of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Plasma Concentration of Intact XTX202 by Nominal Time (h) From End of Infusion Following a Single IV Administration of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=5 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=7 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=4 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=9 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Plasma Concentrations of Intact XTX202
0.250 hours
23100 ng/mL
Standard Deviation 5480
50100 ng/mL
Standard Deviation 13600
76700 ng/mL
Standard Deviation 14400
NA ng/mL
Sample collected at incorrect time
37600 ng/mL
Standard Deviation NA
Not calculated
50900 ng/mL
Standard Deviation 12800
27400 ng/mL
Standard Deviation 4950
85500 ng/mL
Standard Deviation 11900
27800 ng/mL
Standard Deviation 5600
78900 ng/mL
Standard Deviation 14400
NA ng/mL
Below the level of detection
8100 ng/mL
Standard Deviation NA
Not calculated
6450 ng/mL
Standard Deviation 990
15900 ng/mL
Standard Deviation 4350
Plasma Concentrations of Intact XTX202
0.00 hours
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
NA ng/mL
Below the level of detection
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
NA ng/mL
Below the level of detection
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
0 ng/mL
Standard Deviation 0
Plasma Concentrations of Intact XTX202
0.0167 hours
24800 ng/mL
Standard Deviation 6690
45500 ng/mL
Standard Deviation 10800
60400 ng/mL
Standard Deviation 27100
NA ng/mL
Sample collected at incorrect time
49700 ng/mL
Standard Deviation 14700
25900 ng/mL
Standard Deviation 3680
79200 ng/mL
Standard Deviation 10100
25800 ng/mL
Standard Deviation 5690
87700 ng/mL
Standard Deviation 15800
NA ng/mL
Sample collected at incorrect time
6240 ng/mL
Standard Deviation NA
Not calculated
7250 ng/mL
Standard Deviation 1000
19100 ng/mL
Standard Deviation 6280
Plasma Concentrations of Intact XTX202
0.500 hours
23400 ng/mL
Standard Deviation 7840
47600 ng/mL
Standard Deviation 14900
75400 ng/mL
Standard Deviation 16300
NA ng/mL
Sample collected at incorrect time
33200 ng/mL
Standard Deviation NA
Not calculated
47900 ng/mL
Standard Deviation 13000
25500 ng/mL
Standard Deviation 4670
77600 ng/mL
Standard Deviation 11400
27300 ng/mL
Standard Deviation 5360
79200 ng/mL
Standard Deviation 18900
4120 ng/mL
6800 ng/mL
Standard Deviation 1970
6280 ng/mL
Standard Deviation 1120
15100 ng/mL
Standard Deviation 5010
Plasma Concentrations of Intact XTX202
1.50 hours
20800 ng/mL
Standard Deviation 4610
39900 ng/mL
Standard Deviation 14800
68600 ng/mL
Standard Deviation 11900
16000 ng/mL
25700 ng/mL
Standard Deviation 7920
42300 ng/mL
Standard Deviation 9980
22800 ng/mL
Standard Deviation 2760
65700 ng/mL
Standard Deviation 13400
26300 ng/mL
Standard Deviation 6410
63200 ng/mL
Standard Deviation 14000
4300 ng/mL
4600 ng/mL
Standard Deviation 1580
7780 ng/mL
Standard Deviation 2950
12800 ng/mL
Standard Deviation 3850
Plasma Concentrations of Intact XTX202
3.00 hours
19500 ng/mL
Standard Deviation 5180
31100 ng/mL
Standard Deviation 10200
55100 ng/mL
Standard Deviation 1400
13800 ng/mL
22700 ng/mL
Standard Deviation 9620
41300 ng/mL
Standard Deviation 12100
22300 ng/mL
Standard Deviation 636
52800 ng/mL
Standard Deviation 12700
18200 ng/mL
Standard Deviation 7360
65300 ng/mL
Standard Deviation 14900
3430 ng/mL
4320 ng/mL
Standard Deviation 941
6330 ng/mL
Standard Deviation 1280
12500 ng/mL
Standard Deviation 3710
Plasma Concentrations of Intact XTX202
24.0 hours
11800 ng/mL
Standard Deviation 2840
19800 ng/mL
Standard Deviation 5870
32600 ng/mL
Standard Deviation 8050
8360 ng/mL
13100 ng/mL
Standard Deviation 4100
30800 ng/mL
Standard Deviation NA
Not calculated
14900 ng/mL
Standard Deviation NA
Not calculated
25100 ng/mL
Standard Deviation NA
Not calculated
15200 ng/mL
Standard Deviation 5770
2530 ng/mL
3470 ng/mL
Standard Deviation 657
4410 ng/mL
Standard Deviation 887
7240 ng/mL
Standard Deviation 2190
Plasma Concentrations of Intact XTX202
72.0 hours
6660 ng/mL
Standard Deviation 1390
11800 ng/mL
Standard Deviation 4880
18100 ng/mL
Standard Deviation 5710
NA ng/mL
Sample collected at incorrect time
8240 ng/mL
Standard Deviation 2920
14300 ng/mL
Standard Deviation 4340
8420 ng/mL
Standard Deviation 2380
16300 ng/mL
Standard Deviation 3180
8740 ng/mL
Standard Deviation 3170
19000 ng/mL
Standard Deviation 4640
1370 ng/mL
1680 ng/mL
Standard Deviation 28.3
2050 ng/mL
Standard Deviation 191
4270 ng/mL
Standard Deviation 2120
Plasma Concentrations of Intact XTX202
144 hours
4470 ng/mL
Standard Deviation 1080
6850 ng/mL
Standard Deviation 3070
10800 ng/mL
Standard Deviation 3180
3260 ng/mL
6850 ng/mL
Standard Deviation NA
Not calculated
8250 ng/mL
Standard Deviation 2490
5700 ng/mL
Standard Deviation 940
10600 ng/mL
Standard Deviation 3650
5130 ng/mL
Standard Deviation 2110
9370 ng/mL
Standard Deviation 1560
965 ng/mL
1180 ng/mL
Standard Deviation 383
1610 ng/mL
Standard Deviation 369
2790 ng/mL
Standard Deviation 967
Plasma Concentrations of Intact XTX202
312 hours
2330 ng/mL
Standard Deviation 689
4200 ng/mL
Standard Deviation 1910
6250 ng/mL
Standard Deviation 1900
1470 ng/mL
2180 ng/mL
Standard Deviation NA
Not calculated
5440 ng/mL
Standard Deviation 2100
3080 ng/mL
Standard Deviation 841
5510 ng/mL
Standard Deviation 971
3260 ng/mL
Standard Deviation 1370
5440 ng/mL
Standard Deviation 1710
610 ng/mL
759 ng/mL
Standard Deviation 387
1070 ng/mL
Standard Deviation 227
1910 ng/mL
Standard Deviation 679
Plasma Concentrations of Intact XTX202
504 hours
1440 ng/mL
Standard Deviation 312
1880 ng/mL
Standard Deviation 826
3950 ng/mL
Standard Deviation 1300
1190 ng/mL
1540 ng/mL
Standard Deviation NA
Not calculated
2950 ng/mL
Standard Deviation 1310
1790 ng/mL
Standard Deviation 481
3190 ng/mL
Standard Deviation 559
1890 ng/mL
Standard Deviation 1170
2970 ng/mL
Standard Deviation 1370
347 ng/mL
437 ng/mL
Standard Deviation 238
3620 ng/mL
Standard Deviation 5400
922 ng/mL
Standard Deviation 415

SECONDARY outcome

Timeframe: From Cycle 1 to up to Cycle 18 (21 days per cycle)

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Plasma Trough Concentration of Total XTX202 Following Multiple IV Administrations of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=5 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=7 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=5 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=9 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Total XTX202 Plasma Trough Concentration
Cycle 3
1970 ng/mL
Standard Deviation 876
4070 ng/mL
Standard Deviation 2590
4780 ng/mL
Standard Deviation 2000
2030 ng/mL
4260 ng/mL
Standard Deviation 881
2730 ng/mL
Standard Deviation 1080
3810 ng/mL
Standard Deviation 399
2320 ng/mL
Standard Deviation 1140
233 ng/mL
627 ng/mL
Standard Deviation 465
5430 ng/mL
Standard Deviation 9510
1330 ng/mL
Standard Deviation 506
Total XTX202 Plasma Trough Concentration
Cycle 1
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
NA ng/mL
Below the level of detection
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
NA ng/mL
Below the level of detection
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
Total XTX202 Plasma Trough Concentration
Cycle 2
1470 ng/mL
Standard Deviation 338
2070 ng/mL
Standard Deviation 907
3660 ng/mL
Standard Deviation 1500
1180 ng/mL
1480 ng/mL
Standard Deviation NA
Not Calculated
3160 ng/mL
Standard Deviation 1290
1810 ng/mL
Standard Deviation 424
3090 ng/mL
Standard Deviation 233
1950 ng/mL
Standard Deviation 1400
3030 ng/mL
Standard Deviation 1360
363 ng/mL
307 ng/mL
Standard Deviation 80.6
12600 ng/mL
Standard Deviation 22200
1270 ng/mL
Standard Deviation 1170
Total XTX202 Plasma Trough Concentration
Cycle 4
2030 ng/mL
Standard Deviation 1340
2360 ng/mL
Standard Deviation 679
5860 ng/mL
Standard Deviation 2080
4610 ng/mL
Standard Deviation NA
Not Calculated
2500 ng/mL
Standard Deviation 544
5370 ng/mL
Standard Deviation 6630
293 ng/mL
Standard Deviation NA
Not Calculated
4230 ng/mL
Standard Deviation 5780
1530 ng/mL
Standard Deviation 992
Total XTX202 Plasma Trough Concentration
Cycle 5
1690 ng/mL
Standard Deviation 884
6260 ng/mL
Standard Deviation 735
2770 ng/mL
Standard Deviation 742
1070 ng/mL
Standard Deviation 1330
2060 ng/mL
Standard Deviation 2200
1980 ng/mL
Standard Deviation 1310
Total XTX202 Plasma Trough Concentration
Cycle 6
6490 ng/mL
Standard Deviation NA
Not Calculated
3120 ng/mL
Standard Deviation 912
1840 ng/mL
Standard Deviation NA
Not Calculated
1080 ng/mL
Standard Deviation 277
2110 ng/mL
Standard Deviation NA
Not Calculated
Total XTX202 Plasma Trough Concentration
Cycle 7
1140 ng/mL
Standard Deviation 330
Total XTX202 Plasma Trough Concentration
Cycle 8
1150 ng/mL
Standard Deviation 335
Total XTX202 Plasma Trough Concentration
Cycle 9
1490 ng/mL
Standard Deviation 643
Total XTX202 Plasma Trough Concentration
Cycle 12
1120 ng/mL
Standard Deviation NA
Not Calculated
Total XTX202 Plasma Trough Concentration
Cycle 15
2230 ng/mL
Standard Deviation 431
Total XTX202 Plasma Trough Concentration
Cycle 18
2180 ng/mL
Standard Deviation 7.07

SECONDARY outcome

Timeframe: from Cycle 1 to up to Cycle 18 (21 days per cycle)

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Plasma Trough Concentration of Intact XTX202 Following Multiple IV Administrations of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=5 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=7 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=5 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=9 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Intact XTX202 Plasma Trough Concentration
Cycle 1
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
NA ng/mL
Below the level of detection
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
NA ng/mL
Below the level of detection
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
0.00 ng/mL
Standard Deviation 0.00
Intact XTX202 Plasma Trough Concentration
Cycle 2
1440 ng/mL
Standard Deviation 328
1910 ng/mL
Standard Deviation 820
3700 ng/mL
Standard Deviation 1470
1190 ng/mL
1540 ng/mL
Standard Deviation NA
Not Calculated
2950 ng/mL
Standard Deviation 1310
1790 ng/mL
Standard Deviation 481
3190 ng/mL
Standard Deviation 559
1890 ng/mL
Standard Deviation 1170
2970 ng/mL
Standard Deviation 1370
347 ng/mL
303 ng/mL
Standard Deviation 76.4
2260 ng/mL
Standard Deviation 4250
861 ng/mL
Standard Deviation 391
Intact XTX202 Plasma Trough Concentration
Cycle 3
1920 ng/mL
Standard Deviation 867
4060 ng/mL
Standard Deviation 2690
4810 ng/mL
Standard Deviation 2090
1760 ng/mL
4260 ng/mL
Standard Deviation 768
2340 ng/mL
Standard Deviation 764
3830 ng/mL
Standard Deviation 557
2340 ng/mL
Standard Deviation 1200
242 ng/mL
621 ng/mL
Standard Deviation 437
671 ng/mL
Standard Deviation 115
1320 ng/mL
Standard Deviation 479
Intact XTX202 Plasma Trough Concentration
Cycle 4
2000 ng/mL
Standard Deviation 1300
2300 ng/mL
Standard Deviation 608
6050 ng/mL
Standard Deviation 2730
4680 ng/mL
Standard Deviation NA
Not Calculated
2540 ng/mL
Standard Deviation 537
5380 ng/mL
Standard Deviation 6560
280 ng/mL
Standard Deviation NA
Not Calculated
852 ng/mL
Standard Deviation 140
1550 ng/mL
Standard Deviation 1010
Intact XTX202 Plasma Trough Concentration
Cycle 5
1770 ng/mL
Standard Deviation 1030
6230 ng/mL
Standard Deviation 997
2720 ng/mL
Standard Deviation 806
1080 ng/mL
Standard Deviation 1340
742 ng/mL
Standard Deviation 162
1940 ng/mL
Standard Deviation 1210
Intact XTX202 Plasma Trough Concentration
Cycle 6
6340 ng/mL
Standard Deviation NA
Not Calculated
3220 ng/mL
Standard Deviation 1030
1870 ng/mL
Standard Deviation NA
Not Calculated
1100 ng/mL
Standard Deviation 346
2080 ng/mL
Standard Deviation NA
Not Calculated
Intact XTX202 Plasma Trough Concentration
Cycle 7
1160 ng/mL
Standard Deviation 356
Intact XTX202 Plasma Trough Concentration
Cycle 8
1110 ng/mL
Standard Deviation 367
Intact XTX202 Plasma Trough Concentration
Cycle 9
1420 ng/mL
Standard Deviation 453
Intact XTX202 Plasma Trough Concentration
Cycle 12
1090 ng/mL
Standard Deviation NA
Not Calculated
Intact XTX202 Plasma Trough Concentration
Cycle 15
2240 ng/mL
Standard Deviation 474
Intact XTX202 Plasma Trough Concentration
Cycle 18
2020 ng/mL
Standard Deviation 346

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Cmax following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=5 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=7 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Maximum Observed Plasma Concentration (Cmax) of Total XTX202
27700 ng/mL
Standard Deviation 6790
45700 ng/mL
Standard Deviation 14800
80300 ng/mL
Standard Deviation 17400
17200 ng/mL
32500 ng/mL
Standard Deviation 9620
51800 ng/mL
Standard Deviation 13200
30900 ng/mL
Standard Deviation 3180
76500 ng/mL
Standard Deviation 14200
31400 ng/mL
Standard Deviation 7460
84400 ng/mL
Standard Deviation 15500
4410 ng/mL
7130 ng/mL
Standard Deviation 1540
8400 ng/mL
Standard Deviation 1590
18500 ng/mL
Standard Deviation 6140

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Cmax following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=5 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=7 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=4 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=9 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Maximum Observed Plasma Concentration (Cmax) of Intact XTX202
27300 ng/mL
Standard Deviation 6920
45800 ng/mL
Standard Deviation 14700
80600 ng/mL
Standard Deviation 17700
18400 ng/mL
31400 ng/mL
Standard Deviation 8770
52200 ng/mL
Standard Deviation 14100
29700 ng/mL
Standard Deviation 1700
80800 ng/mL
Standard Deviation 16800
31400 ng/mL
Standard Deviation 7670
85600 ng/mL
Standard Deviation 16000
4300 ng/mL
6810 ng/mL
Standard Deviation 1200
9550 ng/mL
Standard Deviation 2740
18300 ng/mL
Standard Deviation 5780

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results. Note: In Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg Arm, Tmax value for Cycle 1 was reported based on measured concentration at collection timepoint scheduled immediately prior to Cycle 2 dose, however this collection timepoint may have been taken following the second dose

Time of maximum observed concentration (Tmax) of total XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=5 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=7 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Time of Maximum Observed Concentration (Tmax) of Total XTX202
0.658 h
Standard Deviation 0.213
0.981 h
Standard Deviation 0.467
0.817 h
Standard Deviation 0.163
0.98 h
0.708 h
Standard Deviation 0.0589
0.647 h
Standard Deviation 0.113
0.650 h
Standard Deviation 0.212
1.06 h
Standard Deviation 0.768
0.806 h
Standard Deviation 0.213
1.15 h
Standard Deviation 0.323
2.05 h
1.00 h
Standard Deviation 0.0726
168 h
Standard Deviation 291
0.710 h
Standard Deviation 0.332

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results. Note: In Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg Arm, Tmax value for Cycle 1 was reported based on measured concentration at collection timepoint scheduled immediately prior to Cycle 2 dose, however this collection timepoint may have been taken following the second dose.

Time of maximum observed concentration (Tmax) of intact XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=5 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=7 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=4 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=9 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Time of Maximum Observed Concentration (Tmax) of Intact XTX202
0.680 h
Standard Deviation 0.258
1.05 h
Standard Deviation 0.403
0.838 h
Standard Deviation 0.170
0.98 h
0.783 h
Standard Deviation 0.0471
0.694 h
Standard Deviation 0.107
0.650 h
Standard Deviation 0.212
1.00 h
Standard Deviation 0.796
0.761 h
Standard Deviation 0.225
1.15 h
Standard Deviation 0.129
2.05 h
1.00 h
Standard Deviation 0.0726
126 h
Standard Deviation 252
0.694 h
Standard Deviation 0.311

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results

Area under the curve (AUC)of total XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=3 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Area Under the Curve From Time 0 to 504 Hours (AUC0-504) of Total XTX202
2310000 h*ng/mL
Standard Deviation 423000
3770000 h*ng/mL
Standard Deviation 1600000
5720000 h*ng/mL
Standard Deviation 1590000
1490000 h*ng/mL
2670000 h*ng/mL
Standard Deviation 938000
4670000 h*ng/mL
Standard Deviation 1390000
2760000 h*ng/mL
Standard Deviation 467000
5380000 h*ng/mL
Standard Deviation 651000
2610000 h*ng/mL
Standard Deviation 768000
6170000 h*ng/mL
Standard Deviation 1970000
479000 h*ng/mL
653000 h*ng/mL
Standard Deviation 190000
1050000 h*ng/mL
Standard Deviation 477000
1490000 h*ng/mL
Standard Deviation 478000

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results

Area under the curve (AUC) of intact XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=7 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=6 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=3 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=4 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=9 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Area Under the Curve From Time 0 to 504 Hours (AUC0-504) of Intact XTX202
2160000 h*ng/mL
Standard Deviation 382000
3630000 h*ng/mL
Standard Deviation 1480000
5810000 h*ng/mL
Standard Deviation 1590000
1500000 h*ng/mL
2630000 h*ng/mL
Standard Deviation 991000
4680000 h*ng/mL
Standard Deviation 1370000
2760000 h*ng/mL
Standard Deviation 484000
5410000 h*ng/mL
Standard Deviation 941000
2580000 h*ng/mL
Standard Deviation 800000
6190000 h*ng/mL
Standard Deviation 2020000
469000 h*ng/mL
639000 h*ng/mL
Standard Deviation 203000
1010000 h*ng/mL
Standard Deviation 404000
1440000 h*ng/mL
Standard Deviation 501000

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results

Half-life (T1/2) of total XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=9 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=10 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=1 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=4 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=3 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=2 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=2 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=5 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Half-life (T1/2) of Total XTX202
187 h
Standard Deviation 17.5
207 h
Standard Deviation 81.1
189 h
Standard Deviation 31.0
NA h
Sampling duration is insufficient for calculation
182 h
Standard Deviation NA
Not Calculated
185 h
Standard Deviation 36.1
203 h
Standard Deviation 0.813
213 h
Standard Deviation 19.6
192 h
Standard Deviation 53.4
167 h
Standard Deviation 59.7
NA h
Sampling duration is insufficient for calculation
200 h
Standard Deviation 23.8
207 h
Standard Deviation 26.4
238 h
Standard Deviation 43.8

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results

Half-life (T1/2) of intact XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=9 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=9 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=1 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=3 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=2 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=2 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=7 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Half-life (T1/2) of Intact XTX202
192 h
Standard Deviation 17.6
205 h
Standard Deviation 81.3
179 h
Standard Deviation 26.7
NA h
Sampling duration is insufficient for calculation
185 h
Standard Deviation NA
Not Calculated
183 h
Standard Deviation 29.8
204 h
Standard Deviation 13.1
252 h
Standard Deviation 27.3
212 h
Standard Deviation 57.7
162 h
Standard Deviation 52.4
NA h
Sampling duration is insufficient for calculation
210 h
Standard Deviation 45.2
208 h
Standard Deviation 22.0
229 h
Standard Deviation 40.8

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Systemic clearance (CL) of Total XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=9 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=10 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=1 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=4 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=3 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=2 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=2 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=5 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Systemic Clearance (CL) of Total XTX202
0.0406 L/h
Standard Deviation 0.00625
0.0537 L/h
Standard Deviation 0.0286
0.0534 L/h
Standard Deviation 0.0125
NA L/h
Sampling duration is insufficient for calculation
0.0537 L/h
Standard Deviation NA
Not Calculated
0.0421 L/h
Standard Deviation 0.00730
0.0368 L/h
Standard Deviation 0.00141
0.0404 L/h
Standard Deviation 0.00424
0.0421 L/h
Standard Deviation 0.00856
0.0341 L/h
Standard Deviation 0.00414
NA L/h
Sampling duration is insufficient for calculation
0.0461 L/h
Standard Deviation 0.00774
0.0487 L/h
Standard Deviation 0.00284
0.0418 L/h
Standard Deviation 0.0187

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Systemic clearance (CL) of intact XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=9 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=9 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=1 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=3 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=2 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=2 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=7 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Systemic Clearance (CL) of Intact XTX202
0.0426 L/h
Standard Deviation 0.00569
0.0556 L/h
Standard Deviation 0.0288
0.0526 L/h
Standard Deviation 0.0119
NA L/h
sampling duration is insufficient for calculation
0.0533 L/h
Standard Deviation NA
Not Calculated
0.0454 L/h
Standard Deviation 0.00993
0.0369 L/h
Standard Deviation 0.00216
0.0391 L/h
Standard Deviation 0.00152
0.0419 L/h
Standard Deviation 0.0104
0.0340 L/h
Standard Deviation 0.00443
NA L/h
sampling duration is insufficient for calculation
0.0475 L/h
Standard Deviation 0.00769
0.0489 L/h
Standard Deviation 0.00269
0.0418 L/h
Standard Deviation 0.0184

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Volume of distribution (Vd) of total XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=9 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=10 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=1 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=4 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=3 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=2 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=2 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=5 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Volume of Distribution (Vd) of Total XTX202
10.8 L
Standard Deviation 1.00
13.7 L
Standard Deviation 4.22
14.5 L
Standard Deviation 3.84
NA L
sampling duration is insufficient for calculation
14.1 L
Standard Deviation NA
Not Calculated
11.1 L
Standard Deviation 1.95
10.8 L
Standard Deviation 0.370
12.5 L
Standard Deviation 2.45
11.3 L
Standard Deviation 1.85
8.37 L
Standard Deviation 3.93
NA L
sampling duration is insufficient for calculation
13.2 L
Standard Deviation 0.648
14.6 L
Standard Deviation 2.70
13.5 L
Standard Deviation 4.35

SECONDARY outcome

Timeframe: up to 21 days following a single IV infusion of XTX202 on Cycle 1

Population: Participants received at least one dose of XTX202 and had at least 1 post dose measurement of XTX202 without protocol deviations or events affecting the validity of the PK results.

Volume of distribution (Vd) of intact XTX202 following a single IV infusion of XTX202. In the analysis set used for PK, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=9 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=9 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=1 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=3 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=2 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=2 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=2 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=7 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Volume of Distribution (Vd) of Intact XTX202
11.7 L
Standard Deviation 1.32
14.0 L
Standard Deviation 4.02
13.7 L
Standard Deviation 3.96
NA L
Sampling duration is insufficient for calculation
14.2 L
Standard Deviation NA
Not Calculated
11.9 L
Standard Deviation 2.89
10.8 L
Standard Deviation 0.0580
14.2 L
Standard Deviation 2.09
12.3 L
Standard Deviation 1.35
8.11 L
Standard Deviation 3.61
NA L
Sampling duration is insufficient for calculation
14.1 L
Standard Deviation 0.767
14.8 L
Standard Deviation 2.36
13.2 L
Standard Deviation 4.94

SECONDARY outcome

Timeframe: from Cycle 1 Day 1 to up to 24 months

Population: Participants who received at least one dose of XTX202 and had at least one post baseline blood sample collected to assess immunogenicity with reportable result.

Overall ADA Incidence Following a Single IV Administration of XTX202 In the analysis set used for ADA, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 1 Part 1B initially received XTX202 2.8 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=11 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=12 Participants
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 Participants
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=6 Participants
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=5 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=9 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Antidrug Antibody (ADA) Occurrence and Titer in Serum (Phase 1 Only)
5 Participants
3 Participants
1 Participants
0 Participants
0 Participants
1 Participants
0 Participants
0 Participants
1 Participants
3 Participants
4 Participants

SECONDARY outcome

Timeframe: From Cycle 1 Day 1 to up to 24 months

Population: Participants who received at least one dose of XTX202 and had at least one post baseline blood sample collected to assess immunogenicity with reportable result.

Overall ADA Incidence Following a Single IV Administration of XTX202. In the analysis set used for ADA, participants are assigned to a treatment group based on the initial dose received. In the Participant Flow module, participants are assigned to a treatment group based on the highest dose received. One participant in Phase 2 Part 2B initially received XTX202 1.4 mg/kg, then increased the dose to 4.0 mg/kg at a later cycle and was therefore included in the XTX202 4.0 mg/kg dose group.

Outcome measures

Outcome measures
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=2 Participants
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=15 Participants
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=6 Participants
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=13 Participants
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Incidence and Persistence of ADAs (Including Neutralizing ADAs) and Titers (Phase 2 Only)
0 Participants
0 Participants
1 Participants
0 Participants

Adverse Events

Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg

Serious events: 0 serious events
Other events: 1 other events
Deaths: 1 deaths

Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg

Serious events: 0 serious events
Other events: 1 other events
Deaths: 2 deaths

Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg

Serious events: 0 serious events
Other events: 2 other events
Deaths: 3 deaths

Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg

Serious events: 0 serious events
Other events: 6 other events
Deaths: 6 deaths

Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg

Serious events: 0 serious events
Other events: 10 other events
Deaths: 11 deaths

Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg

Serious events: 0 serious events
Other events: 7 other events
Deaths: 6 deaths

Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg

Serious events: 4 serious events
Other events: 12 other events
Deaths: 5 deaths

Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg

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

Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg

Serious events: 0 serious events
Other events: 2 other events
Deaths: 2 deaths

Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg

Serious events: 0 serious events
Other events: 3 other events
Deaths: 2 deaths

Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg

Serious events: 0 serious events
Other events: 1 other events
Deaths: 0 deaths

Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg

Serious events: 0 serious events
Other events: 2 other events
Deaths: 0 deaths

Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg

Serious events: 6 serious events
Other events: 15 other events
Deaths: 0 deaths

Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg

Serious events: 2 serious events
Other events: 5 other events
Deaths: 1 deaths

Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg

Serious events: 2 serious events
Other events: 14 other events
Deaths: 6 deaths

Serious adverse events

Serious adverse events
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 participants at risk
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 participants at risk
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 participants at risk
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 participants at risk
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 participants at risk
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 participants at risk
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 participants at risk
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 participants at risk
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 participants at risk
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 participants at risk
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
n=1 participants at risk
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 participants at risk
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=15 participants at risk
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=5 participants at risk
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=15 participants at risk
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Hepatobiliary disorders
Hypertransaminasaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Immune system disorders
Cytokine release syndrome
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Immune system disorders
Immune system disorder
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Colitis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Renal and urinary disorders
Acute kidney injury
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Pleural effusion
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Hepatobiliary disorders
Autoimmune hepatitis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Hepatobiliary disorders
Hyperbilirubinaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Dyspnoea
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Hypoxia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
General disorders
Pyrexia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Injury, poisoning and procedural complications
infusion related reaction
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Dizziness
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Lethargy
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Neuropathy peripheral
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Peripheral motor neuropathy
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Polyradiculoneuropathy
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).

Other adverse events

Other adverse events
Measure
Phase 1 Part 1A, Dose Escalation- XTX202 0.27 mg/kg
n=1 participants at risk
XTX202 0.27 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.38 mg/kg
n=3 participants at risk
XTX202 0.38 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 0.53 mg/kg
n=3 participants at risk
XTX202 0.53 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.0 mg/kg
n=8 participants at risk
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 1.4 mg/kg
n=13 participants at risk
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 2.8 mg/kg
n=8 participants at risk
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1A, Dose Escalation- XTX202 4.0 mg/kg
n=13 participants at risk
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.0 mg/kg
n=1 participants at risk
XTX202 1.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 1.4 mg/kg
n=2 participants at risk
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 2.8 mg/kg
n=5 participants at risk
XTX202 2.8 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months
Phase 1 Part 1B, Pharmacodynamics Expansion- XTX202 4.0 mg/kg
n=1 participants at risk
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 1.4 mg/kg
n=2 participants at risk
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2A, Dose Expansion, RCC- XTX202 4.0 mg/kg
n=15 participants at risk
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 1.4 mg/kg
n=5 participants at risk
XTX202 1.4 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
Phase 2 Part 2B, Dose Expansion, Melanoma- XTX202 4.0 mg/kg
n=15 participants at risk
XTX202 4.0 mg/kg was administered on Day 1 of each 21-day cycle for up to 24 months.
General disorders
Fatigue
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
33.3%
1/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
37.5%
3/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
23.1%
3/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
37.5%
3/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
23.1%
3/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
40.0%
2/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
46.7%
7/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
40.0%
2/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
53.3%
8/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
General disorders
Chills
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
37.5%
3/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
69.2%
9/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
60.0%
3/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
2/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
40.0%
6/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
46.7%
7/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
General disorders
Pyrexia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
4/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
61.5%
8/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
33.3%
5/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
26.7%
4/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
General disorders
Oedema peripheral
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
3/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
General disorders
Influenza like illness
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
General disorders
Asthenia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
General disorders
Malaise
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
General disorders
Pain
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Vomiting
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
40.0%
6/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Diarrhoea
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
3/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Nausea
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Dry mouth
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Oral pain
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Abdominal distension
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Abdominal pain
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Colitis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Gastrooesophageal reflux disease
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Lip swelling
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Stomatitis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Swollen tongue
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Rash
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
3/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Rash maculo-papular
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Dermatitis acneiform
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Hyperhidrosis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Pruritus
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
33.3%
1/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Blister
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Rash vesicular
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Urticaria
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Alanine aminotransferase increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
3/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Aspartate aminotransferase increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
40.0%
2/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Lymphocyte count decreased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
33.3%
1/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
23.1%
3/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
25.0%
2/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Blood alkaline phosphatase increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
3/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Lipase increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Lymphocyte count increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Neutrophil count decreased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
40.0%
2/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Platelet count decreased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
White blood cell count decreased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Blood bilirubin increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Blood lactic acid increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Blood thyroid stimulating hormone increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
C-reactive protein increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Haemoglobin increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Metabolism and nutrition disorders
Hypomagnesaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
International normalised ratio increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Metabolism and nutrition disorders
Decreased appetite
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
26.7%
4/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Metabolism and nutrition disorders
Hyperglycaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Metabolism and nutrition disorders
Hyperkalaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Metabolism and nutrition disorders
Hyponatraemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Metabolism and nutrition disorders
Hypercalcaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Metabolism and nutrition disorders
Hypophosphataemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Dizziness
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
33.3%
1/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Headache
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
33.3%
1/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Peripheral motor neuropathy
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Peripheral sensory neuropathy
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Lethargy
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Neuropathy peripheral
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Polyradiculoneuropathy
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Nervous system disorders
Presyncope
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Infections and infestations
Rash pustular
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
26.7%
4/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Musculoskeletal and connective tissue disorders
Myalgia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
25.0%
2/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Musculoskeletal and connective tissue disorders
Muscle spasms
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Musculoskeletal and connective tissue disorders
Muscular weakness
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Musculoskeletal and connective tissue disorders
Pain in extremity
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Blood and lymphatic system disorders
Anaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Blood and lymphatic system disorders
Thrombocytopenia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Blood and lymphatic system disorders
Leukocytosis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Blood and lymphatic system disorders
Neutropenia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Acute respiratory failure
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Cough
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
50.0%
1/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Dyspnoea
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Hypoxia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Pleural effusion
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Cardiac disorders
Atrial fibrillation
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Cardiac disorders
Sinus tachycardia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Hepatobiliary disorders
Hypertransaminasaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
3/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Immune system disorders
Cytokine release syndrome
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Immune system disorders
Immune system disorder
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Vascular disorders
Hypotension
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
13.3%
2/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Endocrine disorders
Adrenal insufficiency
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Eye disorders
Glaucoma
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Injury, poisoning and procedural complications
Infusion related reaction
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Psychiatric disorders
Confusional state
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Renal and urinary disorders
Acute kidney injury
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
6.7%
1/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Amylase increased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Weight decreased
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Skin hypopigmentation
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Vitiligo
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
20.0%
1/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Musculoskeletal and connective tissue disorders
Back pain
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Musculoskeletal and connective tissue disorders
Tendon pain
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Vascular disorders
Hypertension
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Constipation
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
33.3%
1/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
15.4%
2/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Abdominal pain upper
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Anal incontinence
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Gastrointestinal disorders
Gastritis
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Investigations
Lymphocyte morphology abnormal
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Blood and lymphatic system disorders
Lymphopenia
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Metabolism and nutrition disorders
Dehydration
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Musculoskeletal and connective tissue disorders
Arthralgia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Musculoskeletal and connective tissue disorders
Immune-mediated arthritis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Night Sweats
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Skin and subcutaneous tissue disorders
Subcorneal pustular dermatosis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Infections and infestations
Soft tissue infection
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Infections and infestations
Vulval abscess
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Respiratory, thoracic and mediastinal disorders
Nasal congestion
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Hepatobiliary disorders
Hyperbilirubinaemia
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Hepatobiliary disorders
Autoimmune hepatitis
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Hepatobiliary disorders
Drug-induced liver injury
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Vascular disorders
Hot flush
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Endocrine disorders
Hypothyroidism
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
12.5%
1/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
Tumor pain
100.0%
1/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
Renal and urinary disorders
Renal failure
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/3 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/8 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
7.7%
1/13 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/1 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/2 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/5 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).
0.00%
0/15 • Participants were assessed for All-Cause Mortality from their first dose until the study was completed (up to approximately 24 months). Treatment-emergent related SAEs and Other related AEs were assessed from first dose to 90 days post last dose (up to approximately 24 months).

Additional Information

Xilio Medical Affairs

Xilio Development, Inc.

Phone: 857-524-2466

Results disclosure agreements

  • Principal investigator is a sponsor employee
  • Publication restrictions are in place