Trial Outcomes & Findings for A Study to Learn About Lorlatinib in Patients With Non-Small Cell Lung Cancer Which Could Not Be Controlled (NCT NCT06282991)
NCT ID: NCT06282991
Last Updated: 2026-03-10
Results Overview
Number of participants according to first line therapy treatment pattern was reported in this outcome measure.
Recruitment status
COMPLETED
Target enrollment
73 participants
Primary outcome timeframe
Baseline; data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Results posted on
2026-03-10
Participant Flow
Participants who were treated with Lorlatinib for advanced non-small cell lung cancer (NSCLC), progressed on first- or second- generation tyrosine kinase inhibitor (TKI) and who had participated in Lorlatinib compassionate use program (CUP) were observed in this study at the physician's discretion.
Participant milestones
| Measure |
Lorlatinib
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
|
Overall Study
STARTED
|
73
|
|
Overall Study
COMPLETED
|
73
|
|
Overall Study
NOT COMPLETED
|
0
|
Reasons for withdrawal
Withdrawal data not reported
Baseline Characteristics
Race and Ethnicity were not collected from any participant.
Baseline characteristics by cohort
| Measure |
Lorlatinib
n=73 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Age, Continuous
|
51.9 Years
STANDARD_DEVIATION 12.5 • n=73 Participants
|
|
Sex: Female, Male
Female
|
39 Participants
n=73 Participants
|
|
Sex: Female, Male
Male
|
34 Participants
n=73 Participants
|
PRIMARY outcome
Timeframe: Baseline; data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Analysis population included all eligible participants whose data were observed in the study.
Number of participants according to first line therapy treatment pattern was reported in this outcome measure.
Outcome measures
| Measure |
Lorlatinib
n=73 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Number of Participants According to First Line Therapy Treatment Pattern From Initial Diagnosis to Current Lorlatinib Treatment
Single TKI
|
25 Participants
|
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Number of Participants According to First Line Therapy Treatment Pattern From Initial Diagnosis to Current Lorlatinib Treatment
Single Chemotherapy
|
3 Participants
|
|
Number of Participants According to First Line Therapy Treatment Pattern From Initial Diagnosis to Current Lorlatinib Treatment
Combination Chemotherapy (2 Agents)
|
40 Participants
|
|
Number of Participants According to First Line Therapy Treatment Pattern From Initial Diagnosis to Current Lorlatinib Treatment
Single TKI + Single Chemotherapy
|
2 Participants
|
|
Number of Participants According to First Line Therapy Treatment Pattern From Initial Diagnosis to Current Lorlatinib Treatment
Combination Chemotherapy (2 Agents) + Single Other
|
3 Participants
|
PRIMARY outcome
Timeframe: From first dose of lorlatinib until 30 Sep 2020 or death whichever occurred first (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Evaluable response analysis set included treated participants who had tumor baseline values and at least one post-baseline tumor assessment and received at least one-month Lorlatinib treatment. Here, 'Overall Number of Participants Analyzed' signifies participants evaluable for this outcome measure. Participants who could not be evaluated did not contribute to data reported below.
ORR was defined as the percentage of participants in whom complete response (CR), or partial response (PR) was observed. According to Response Evaluation Criteria in Solid Tumors (RECIST) v1.1: 1) CR is defined as disappearance of all target lesions or partial response (PR) defined as \>=30 percent (%) decrease in sum of the longest dimensions (LD) of the target lesions taking as a reference the baseline sum LD .
Outcome measures
| Measure |
Lorlatinib
n=60 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Objective Response Rate (ORR) During Lorlatinib Treatment
|
25.0 Percentage of participants
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PRIMARY outcome
Timeframe: From first dose of lorlatinib until date of death or censoring date (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Evaluable response analysis set included treated participants who had tumor baseline values and at least one post-baseline tumor assessment and received at least one-month Lorlatinib treatment.
Overall survival was defined as the time from the date of first dose of lorlatinib to the date of death, censored at the participant's last contact date or the data cutoff date, whichever was earlier. Overall survival was evaluated using Kaplan-Meier method.
Outcome measures
| Measure |
Lorlatinib
n=62 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Overall Survival
|
19.6 Months
Interval 17.2 to 20.3
|
PRIMARY outcome
Timeframe: From first dose of lorlatinib until date of death or censoring date (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Evaluable response analysis set included participants who had tumor baseline values and at least one post-baseline tumor assessment and received at least one-month Lorlatinib treatment.
PFS refers to the duration from the first study treatment of Lorlatinib to the first documentation of disease progression or death or censored date. According to RECIST, progression is defined as at least a 20% increase in the sum of the diameters of target lesions, taking as reference the smallest sum on study. The appearance of one or more new lesions is also considered progression. PFS was evaluated using the Kaplan-Meier method.
Outcome measures
| Measure |
Lorlatinib
n=62 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Progression Free Survival (PFS) For Lorlatinib Treatment
|
15.4 Months
Interval 0.0 to 40.0
|
PRIMARY outcome
Timeframe: 1 year; data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Evaluable response analysis set included treated participants who had tumor baseline values and at least one post-baseline tumor assessment and received at least one-month Lorlatinib treatment.
OS was defined as the time from the date of first dose of lorlatinib to the date of death, censored at the participant's last contact date or the data cutoff date, whichever was earlier. In this outcome measure percentage of participants who survived for 1 year are reported.
Outcome measures
| Measure |
Lorlatinib
n=62 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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1-year OS Rate on Lorlatinib
|
79.0 Percentage of participants
|
PRIMARY outcome
Timeframe: From date of first dose of NSCLC treatment until treatment failure (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Evaluable response analysis set included treated participants who had tumor baseline values and at least one post-baseline tumor assessment and received at least one-month Lorlatinib treatment. Here, 'Overall Number of Participants Analyzed' signifies participants evaluable for this outcome measure.
TTF was defined as duration of first dose of any NSCLC treatment to treatment failure (defined as any discontinuation, including cancer progression, adverse events, or death).
Outcome measures
| Measure |
Lorlatinib
n=60 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Time to Treatment Failure (TTF) for All NSCLC Treatment
|
7.3 Months
Interval 0.0 to 41.1
|
PRIMARY outcome
Timeframe: From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Evaluable response analysis set included participants who had tumor baseline values and at least one post-baseline tumor assessment and received at least one-month Lorlatinib treatment. Here, 'Overall Number of Participants Analyzed' signifies participants evaluable for this outcome measure.
TTF was defined as duration of first dose of lorlatinib treatment to treatment failure (any discontinuation, including cancer progression, adverse events, or death).
Outcome measures
| Measure |
Lorlatinib
n=28 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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TTF for Lorlatinib Treatment Failure
|
6.7 Months
Interval 1.4 to 25.7
|
PRIMARY outcome
Timeframe: From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Safety analysis set included participants who received at least one dose of Lorlatinib.
An ADR is defined as all noxious and unintended responses to a medicinal product related to any dose. Common ADRs were hyperlipidemia, hyperglycemia, rash \& itch, mental disorder, edema, body weight gain, transaminase level escalation, peripheral neuropathy, thrombocytopenia, gastrointestinal disorder, creatine kinase increased, dizziness and pneumonitis. Lorlatinib related ADR was recorded from first dose of Lorlatinib until end of study.
Outcome measures
| Measure |
Lorlatinib
n=73 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Number of Participants With Common Adverse Drug Reaction (ADRs)
Hyperlipidemia
|
43 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Hyperglycemia
|
2 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Rash & itch
|
2 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Mental disorder
|
5 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Edema
|
6 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Body weight gain
|
9 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Transaminase level escalation
|
3 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Peripheral Neuropathy
|
5 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Thrombocytopenia
|
2 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Gastrointestinal disorder
|
2 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Creatine kinase increased
|
1 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Dizziness
|
1 Participants
|
|
Number of Participants With Common Adverse Drug Reaction (ADRs)
Pneumonitis
|
1 Participants
|
PRIMARY outcome
Timeframe: From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Safety analysis set included participants who received at least one dose of Lorlatinib. Here, all participants reported under "Overall Number of Participants Analyzed" contributed data to the table; however, may not be evaluable for each row. "Number analyzed" signifies the number of participants with the specified ADR.
An ADR is defined as all noxious and unintended responses to a medicinal product related to any dose. Common ADRs were hyperlipidemia, hyperglycemia, rash \& itch, mental disorder, edema, body weight gain, transaminase level escalation, peripheral neuropathy and others (thrombocytopenia, gastrointestinal disorder, creatine kinase increased, dizziness, pneumonitis). Lorlatinib related ADR was recorded from first dose of Lorlatinib until end of study. Duration of common ADR is reported in this outcome measure.
Outcome measures
| Measure |
Lorlatinib
n=73 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Duration of Common ADRs
Hyperlipidemia
|
18.1 Months
Standard Deviation 9.9
|
|
Duration of Common ADRs
Hyperglycemia
|
17.9 Months
Standard Deviation 1.9
|
|
Duration of Common ADRs
Rash & itch
|
14.7 Months
Standard Deviation 12.8
|
|
Duration of Common ADRs
Mental disorder
|
17.4 Months
Standard Deviation 10.0
|
|
Duration of Common ADRs
Edema
|
10.8 Months
Standard Deviation 13.4
|
|
Duration of Common ADRs
Body weight gain
|
19.7 Months
Standard Deviation 6.0
|
|
Duration of Common ADRs
Transaminase level escalation
|
3.4 Months
Standard Deviation 5.0
|
|
Duration of Common ADRs
Peripheral Neuropathy
|
8.6 Months
Standard Deviation 10.7
|
|
Duration of Common ADRs
Others
|
19.9 Months
Standard Deviation 3.7
|
PRIMARY outcome
Timeframe: From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Safety analysis set included participants who received at least one dose of Lorlatinib. Here, all participants reported under "Overall Number of Participants Analyzed" contributed data to the table; however, may not be evaluable for each row. "Number analyzed" signifies the number of participants with the specified ADR.
An ADR is defined as all noxious and unintended responses to a medicinal product related to any dose. Number of participants with Grade 1 (mild), Grade 2 (moderate), Grade 3 (severe), Grade 4 (life-threatening) and Unknown were presented in this outcome measure. Severity grades were assessed upon investigator's discretion, wherein grade 1 was minimum severity and grade 4 was maximum severity.
Outcome measures
| Measure |
Lorlatinib
n=73 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
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|---|---|
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Number of Participants According to Severity of Common ADRs
Transaminase level escalation (Grade Unknown)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Peripheral Neuropathy (Grade 1)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Peripheral Neuropathy (Grade 2)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Peripheral Neuropathy (Grade 3)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Peripheral Neuropathy (Grade 4)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Peripheral Neuropathy (Grade Unknown)
|
5 Participants
|
|
Number of Participants According to Severity of Common ADRs
Others (Grade 1)
|
5 Participants
|
|
Number of Participants According to Severity of Common ADRs
Others (Grade 2)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Others (Grade 3)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Transaminase level escalation (Grade 3)
|
2 Participants
|
|
Number of Participants According to Severity of Common ADRs
Transaminase level escalation (Grade 4)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Others (Grade 4)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Others (Grade Unknown)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperlipidemia (Grade 1)
|
12 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperlipidemia (Grade 2)
|
26 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperlipidemia (Grade 3)
|
4 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperlipidemia (Grade 4)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperlipidemia (Grade Unknown)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperglycemia (Grade 1)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperglycemia (Grade 2)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperglycemia (Grade 3)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperglycemia (Grade 4)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Hyperglycemia (Grade Unknown)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Rash & itch (Grade 1)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Rash & itch (Grade 2)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Rash & itch (Grade 3)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Rash & itch (Grade 4)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Rash & itch (Grade Unknown)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Mental disorder (Grade 1)
|
2 Participants
|
|
Number of Participants According to Severity of Common ADRs
Mental disorder (Grade 2)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Mental disorder (Grade 3)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Mental disorder (Grade 4)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Mental disorder (Grade Unknown)
|
3 Participants
|
|
Number of Participants According to Severity of Common ADRs
Edema (Grade 1)
|
5 Participants
|
|
Number of Participants According to Severity of Common ADRs
Edema (Grade 2)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Edema (Grade 3)
|
1 Participants
|
|
Number of Participants According to Severity of Common ADRs
Edema (Grade 4)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Edema (Grade Unknown)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Body weight gain (Grade 1)
|
4 Participants
|
|
Number of Participants According to Severity of Common ADRs
Body weight gain (Grade 2)
|
3 Participants
|
|
Number of Participants According to Severity of Common ADRs
Body weight gain (Grade 3)
|
2 Participants
|
|
Number of Participants According to Severity of Common ADRs
Body weight gain (Grade 4)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Body weight gain (Grade Unknown)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Transaminase level escalation (Grade 1)
|
0 Participants
|
|
Number of Participants According to Severity of Common ADRs
Transaminase level escalation (Grade 2)
|
0 Participants
|
PRIMARY outcome
Timeframe: From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 daysPopulation: Safety analysis set included participants who received at least one dose of Lorlatinib. Here, all participants reported under "Overall Number of Participants Analyzed" contributed data to the table; however, may not be evaluable for each row. "Number analyzed" signifies the number of participants with the specified ADR.
An ADR is defined as all noxious and unintended responses to a medicinal product related to any dose. Participants were categorized as per their ADRs outcome as: recovered, recovered with sequelae (Sequelae refer to any complication or condition that results from a pre-existing illness, injury, or medical intervention), recovering, not recovered, and unknown.
Outcome measures
| Measure |
Lorlatinib
n=73 Participants
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
|
|---|---|
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Number of Participants According to Type of Outcome of Common ADRs
Hyperlipidemia (Recovered)
|
9 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperlipidemia (Recovered with Sequelae)
|
2 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperlipidemia (Recovering)
|
2 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperlipidemia (Not Recovered)
|
29 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperlipidemia (Unknown)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperglycemia (Recovered)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperglycemia (Recovered with Sequelae)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperglycemia (Recovering)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperglycemia (Not Recovered)
|
2 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Hyperglycemia (Unknown)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Rash & Itch (Recovered)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Rash & Itch (Recovered with Sequelae)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Rash & Itch (Recovering)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Rash & Itch (Not Recovered)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Rash & Itch (Unknown)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Mental disorder (Recovered)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Mental disorder (Recovered with Sequelae)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Mental disorder (Recovering)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Mental disorder (Not Recovered)
|
3 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Mental disorder (Unknown)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Edema (Recovered)
|
4 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Edema (Recovered with Sequelae)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Edema (Recovering)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Edema (Not Recovered)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Edema (Unknown)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Body weight gain (Recovered)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Body weight gain (Recovered with Sequelae)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Body weight gain (Recovering)
|
2 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Body weight gain (Not Recovered)
|
7 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Body weight gain (Unknown)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Transaminase level escalation (Recovered)
|
3 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Transaminase level escalation (Recovered with Sequelae)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Transaminase level escalation (Recovering)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Transaminase level escalation (Not Recovered)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Transaminase level escalation (Unknown)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Peripheral Neuropathy (Recovered)
|
3 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Peripheral Neuropathy (Recovered with Sequelae)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Peripheral Neuropathy (Recovering)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Peripheral Neuropathy (Not Recovered)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Peripheral Neuropathy (Unknown)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Others (Recovered)
|
2 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Others (Recovered with Sequelae)
|
0 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Others (Recovering)
|
1 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Others (Not Recovered)
|
2 Participants
|
|
Number of Participants According to Type of Outcome of Common ADRs
Others (Unknown)
|
2 Participants
|
Adverse Events
Lorlatinib
Serious events: 0 serious events
Other events: 41 other events
Deaths: 0 deaths
Serious adverse events
Adverse event data not reported
Other adverse events
| Measure |
Lorlatinib
n=73 participants at risk
Participants (among Taiwanese population) diagnosed with NSCLC who progressed on first- or second- generation TKI chemotherapy and were treated with lorlatinib under real world clinical settings as per physician judgement, were observed in this study. Data was collected from medical records.
|
|---|---|
|
Blood and lymphatic system disorders
Anaemia
|
17.8%
13/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Blood and lymphatic system disorders
Hypereosinophilia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Blood and lymphatic system disorders
Leukopenia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Blood and lymphatic system disorders
Lymph node pain
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Blood and lymphatic system disorders
Neutropenia
|
17.8%
13/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Blood and lymphatic system disorders
Neutrophilia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Blood and lymphatic system disorders
Thrombocytopenia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Cardiac disorders
Congestive heart failure
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Cardiac disorders
Tricuspid insufficiency
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Ear and labyrinth disorders
Tinnitus
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Endocrine disorders
Disorder thyroid
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Abdominal bloating
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Bloody stool
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Constipation
|
4.1%
3/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Diarrhoea
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Gastric ulcer
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Haemorrhoids
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Mucositis oral
|
8.2%
6/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Nausea
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Mouth ulceration
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Toothache
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Gastrointestinal disorders
Ulcer intestinal
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
General disorders
Oedema peripheral
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
General disorders
Oedema
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
General disorders
Fatigue
|
6.8%
5/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
General disorders
Fever
|
4.1%
3/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
General disorders
Mucositis
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
General disorders
Axillary pain
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Hepatobiliary disorders
Jaundice
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Hepatobiliary disorders
Liver disorder
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Immune system disorders
Allergic reaction
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Abscess
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Abscess oral
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Acute gastroenteritis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Acute laryngopharyngitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Acute nasopharyngitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Bronchitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Cellulitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Chronic periodontitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Flu
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Herpes virus infection
|
4.1%
3/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Herpes zoster
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Cellulitis of arm
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Periodontosis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Pneumonia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Septic shock
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Tinea pedis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Tonsillitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Urinary tract infection
|
4.1%
3/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Upper respiratory tract infection
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Injury, poisoning and procedural complications
Dermatitis radiation
|
4.1%
3/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Injury, poisoning and procedural complications
Wound pain
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
Activated partial thromboplastin time prolonged
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
Alanine aminotransferase increased
|
9.6%
7/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
Aspartate aminotransferase increased
|
8.2%
6/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
Blood bilirubin increased
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
Creatinine increased
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
Neutrophil count decreased
|
30.1%
22/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
Platelet count decreased
|
26.0%
19/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
White blood cell count decreased
|
5.5%
4/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Investigations
Weight loss
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Metabolism and nutrition disorders
Decreased appetite
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Metabolism and nutrition disorders
Anorexia
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Metabolism and nutrition disorders
Hypomagnesaemia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Metabolism and nutrition disorders
Hypoalbuminaemia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Metabolism and nutrition disorders
Hypocalcaemia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Musculoskeletal and connective tissue disorders
Muscle soreness
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Musculoskeletal and connective tissue disorders
Arthralgia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Musculoskeletal and connective tissue disorders
Cramp
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Musculoskeletal and connective tissue disorders
Back pain
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Musculoskeletal and connective tissue disorders
Bone pain
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Musculoskeletal and connective tissue disorders
Medication-related osteonecrosis of jaw
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Musculoskeletal and connective tissue disorders
Temporomandibular joint disorder
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Musculoskeletal and connective tissue disorders
Tendon pain
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Nervous system disorders
Dizziness
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Nervous system disorders
Headache
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Nervous system disorders
Numbness of lower extremities
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Psychiatric disorders
Insomnia
|
2.7%
2/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Renal and urinary disorders
Hemorrhagic cystitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Renal and urinary disorders
Hydronephrosis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Respiratory, thoracic and mediastinal disorders
Asthma
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Respiratory, thoracic and mediastinal disorders
Acute respiratory failure
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Respiratory, thoracic and mediastinal disorders
Cough
|
6.8%
5/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Respiratory, thoracic and mediastinal disorders
Pleural effusion
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Respiratory, thoracic and mediastinal disorders
Rhinorrhea
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Respiratory, thoracic and mediastinal disorders
Runny nose
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Respiratory, thoracic and mediastinal disorders
Sore throat
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Respiratory, thoracic and mediastinal disorders
Sputum discolored
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Alopecia
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Bed sore
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Dermatitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Dyshidrosis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Hand and foot syndrome
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Itchy skin
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Ecchymosis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Chronic skin ulcer
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Pruritus
|
4.1%
3/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Psoriasis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Seborrhea capitis
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Skin eruption
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Skin rash
|
4.1%
3/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Itchy rash
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Skin and subcutaneous tissue disorders
Urticaria
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Vascular disorders
Lymphoedema
|
5.5%
4/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Vascular disorders
Raynaud's phenomenon
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Vascular disorders
Hot flashes
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Vascular disorders
Hypertension
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
|
Infections and infestations
Cellulitis of mouth
|
1.4%
1/73 • From date of first dose of lorlatinib until end of study (maximum up to 41.1 months); data retrieved from medical records and observed in this study for approximately 5 months and 28 days
Safety analysis set included participants who received at least one dose of Lorlatinib.
|
Additional Information
Results disclosure agreements
- Principal investigator is a sponsor employee Pfizer has the right to review disclosures, requesting a delay of less than 60 days. Investigator will postpone single center publications until after disclosure of pooled data (all sites), less than 12 months from study completion/termination at all participating sites. Investigator may not disclose previously undisclosed confidential information other than study results.
- Publication restrictions are in place
Restriction type: OTHER