This Study Tests the New Medicine BI 754111 Alone or in C... | NCT03156114 | Trialant
NCT03156114
Sponsor
Boehringer Ingelheim
Status
Completed
Last Update Posted
Jan 26, 2026Actual
Enrollment
172Actual
Phase
Phase 1
Conditions
Neoplasms
Carcinoma, Non-Small-Cell Lung
Interventions
Ezabenlimab
BI 754111
Countries
United States
Canada
Poland
Spain
United Kingdom
Protocol Section
Identification Module
NCT ID
NCT03156114
Obsolete or Duplicate NCT IDs
Not provided
Organization Study
1381-0002
Secondary IDs
ID
Type
Description
Link
2017-005042-29
EudraCT Number
Brief Title
This Study Tests the New Medicine BI 754111 Alone or in Combination With Another New Substance BI 754091 in Patients With Advanced Cancer. The Study Tests Different Doses to Find the Best Dose for Continuous Treatment.
Official Title
An Open Label, Phase I Dose-finding Study of BI 754111 in Combination With BI 754091 in Patients With Advanced Solid Cancers Followed by Expansion Cohorts at the Selected Dose of the Combination in Patients With Non-small Cell Lung Cancer and Other Solid Tumors
Acronym
Not provided
Organization
Boehringer IngelheimINDUSTRY
Status Module
Record Verification Date
Jan 2026
Overall Recruitment Status or Expanded Access Status
Completed
Last Known Status
Not provided
Delayed Posting
Not provided
Why Stopped
Not provided
Expanded Access Info
No
Start Date
Jun 13, 2017Actual
Primary Completion Date
Mar 9, 2023Actual
Completion Date
Jun 6, 2023Actual
First Submitted Date
May 15, 2017
First Submission Date that Met QC Criteria
May 15, 2017
First Posted Date
May 17, 2017Actual
Results Waived
Not provided
Results First Submitted Date
Dec 3, 2025
Results First Submitted that Met QC Criteria
Jan 7, 2026
Results First Posted Date
Jan 26, 2026Actual
Certification/Extension (aka Delayed Results) First Submitted Date
Not provided
Certification/Extension First Submitted that Passed QC Review
Not provided
Certification/Extension First Posted Date
Not provided
Last Update Submitted Date
Jan 7, 2026
Last Update Posted Date
Jan 26, 2026Actual
Sponsor/Collaborators Module
Responsible Party, by Official Title
Sponsor
Lead Sponsor
Boehringer IngelheimINDUSTRY
Collaborators
Not provided
Oversight Module
Has Data Monitoring Committee (DMC)
No
Is FDA Regulated Drug
Yes
Is FDA Regulated Device
No
Is Unapproved Device
Not provided
Pediatric Postmarket Surveillance of a Device Product
Not provided
Product Exported from US
Not provided
FDAAA801 Violation
Not provided
Description Module
Brief Summary
This is a study in adults with advanced solid tumors including non-small cell lung cancer.
The study tests the combination of two medicines called BI 754111 and BI 754091 that may help the immune system to fight the cancer. Such medicines are called immune checkpoint inhibitors.
The study has two parts. In the first part, doctors want to find out the highest dose of 2 medicines that people with solid tumors can tolerate. This dose is then used for the second part of the study.
In the second part, the combination of the two medicines is tested in patients with non-small cell lung cancer and other types of solid cancer. These patients had gotten treatment with anti-PD-1 or anti-PD-L1 medicines but their tumors have come back. The doctors check whether the combination of BI 754111 and BI 754091 makes tumors shrink.
Both medicines are given as an infusion into the vein every 3 weeks. If there is benefit for the patients and if they can tolerate it, the treatment is given for maximum of 1 year. During the entire study doctors will regularly check the health of the patients.
Dose Escalation: Maximum-tolerated Dose (MTD) of the BI 754111 Plus Ezabenlimab Combination
The MTD is defined as the highest dose with less than 25% risk of the true Dose-limiting toxicity (DLT) rate being above 33%. DLTs include:
Haematologic toxicities:
Any Grade 5 toxicity
Neutropenia ≥ Grade 4 for >5 days
Any duration febrile neutropenia
Grade 4 thrombocytopenia or Grade 3 with bleeding/platelet transfusion need
Unexplained Grade 4 anaemia.
Non-haematological toxicities:
Aspartate aminotransferase (AST) or Alanine aminotransferase (ALT) >3x Upper limit of normal (ULN) and total bilirubin >2x ULN without cholestasis signs
≥Grade 4 AST or ALT of any duration
Any ≥Grade 3 non-haematologic toxicity with exceptions
Any Grade 4 or 5 adverse event (AE)
Any Grade 2 pneumonitis
Any Grade 2 uveitis, eye pain, or blurred vision not improving to Grade 1 within 2 weeks or requiring systemic treatment
Any ≥ Grade 2 toxicity causing inability to administer BI 754091 on Cycle 2 Day 1.
First treatment cycle, the first 21 days following the start of trial medication.
Dose Escalation: Number of Patients Experiencing DLTs During the Combination MTD Evaluation Period
Number of patients experiencing DLTs during the combination MTD evaluation period (first cycle of BI 754111 plus ezabenlimab combination therapy) in patients with solid tumours.
First treatment cycle, the first 21 days following the start of trial medication.
Dose Expansion: Number of Patients With Objective Response (OR) - Confirmed Complete Response (CR) and Partial Response (PR)
Dose expansion: Number of patients with objective response (OR) - confirmed complete response (CR) and partial response (PR) according to Response Evaluation Criteria in Solid Tumours (RECIST) Version 1.1 as assessed by the Investigator during the entire treatment.
Complete Response (CR): Disappearance of all target lesions. Any pathological lymph nodes (whether target or non-target) must have reduction in short axis to <10 millimeter.
Partial Response (PR): At least a 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters.
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 818 days.
Secondary Outcomes
Measure
Description
Time Frame
Dose Escalation: Number of Patients With Objective Response (OR) - Confirmed Complete Response (CR) and Partial Response (PR)
Dose escalation: Number of patients with objective response (OR) - confirmed complete response (CR) and partial response (PR) according to RECIST Version 1.1 as assessed by the Investigator during the entire treatment.
Complete Response (CR): Disappearance of all target lesions. Any pathological lymph nodes (whether target or non-target) must have reduction in short axis to <10 millimeter.
Partial Response (PR): At least a 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters.
Other Outcomes
Not provided
Eligibility Module
Eligibility Criteria
Inclusion Criteria:
Provision of signed and dated, written Informed consent form (ICF) prior to any trial-specific procedures, sampling, or analyses
Patients ≥18 years of age at the time of signature of the ICF
Part I (dose escalation):
--Patients with a confirmed diagnosis of advanced, unresectable, and/or metastatic solid tumours (any type)
For whom no therapy of proven efficacy exists, or who are not amenable to standard therapies.
Must have measurable lesions according to Response Evaluation Criteria in Solid Tumours (RECIST) v1.1
Previous treatment with an anti-programmed cell death 1 (receptor) (PD-1) monoclonal antibody (mAb) is allowed as long as the last administration of the anti-PD-1 mAb on the previous treatment is a minimum of 60 days prior to starting treatment in this trial.
Part II (dose expansion):
Patients must have measurable disease per RECIST v1.1 criteria, must have at least 1 tumour lesion amenable to biopsy, and must be medically fit and willing to undergo a biopsy before first treatment (if adequate archival tissue is not available) and, unless clinically contraindicated, after 6 weeks on therapy.
Dose Expansion Cohorts: Patients with a confirmed diagnosis of advanced, unresectable, and/or metastatic solid tumours of one of the following types:
Second and 3rd line Non-small cell lung cancer (NSCLC) patients:
Must have progressed on anti-PD-1 or anti-programmed cell death ligand 1 (PD-L1) treatment after having achieved radiologically confirmed benefit (minimum of stable disease)
Must have had a minimum duration of benefit of 4 months and minimum treatment duration of 2 months on the previous anti- PD-1 or anti-PD-L1 treatment without experiencing disease progression during that period.
The anti-PD-1- or anti-PD-L1-containing treatment must have been the latest treatment regimen prior to enrolling in this trial
Must be within >4 and <12 weeks since the latest treatment and their first dose in this trial. Patients who have had anti-PD-1 or anti-PD-L1 monotherapy as their first-line NSCLC treatment regimen must have a PD-L1 expression level of ≥1% at baseline (local validated testing).
Anti-PD-1 or anti-PD-L1 treatment-naïve patients with microsatellite stable Metastatic colorectal Cancer (mCRC):
Patients must have had ≥ 1 line treatment
Must have microsatellite stable disease (identified using any validated test)
Must be anti-PD-1 and anti-PD-L1 treatment naïve
Anti-PD-1 or anti-PD-L1 pretreated patients with any high Tumour mutational burden (TMB) (≥10 mutations/Mb) and/or Microsatellite instability high (MSI-H) and/or DNA MMRd solid tumours
Patients must have high TMB (≥ 10 mutations/Mb) and/or MSI-H and/or DNA mismatch repair deficient (MMRd) (measured using any validated test).
Patients must have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
1st-line squamous or non-squamous NSCLC patients:
Patients must be treatment naïve
Must be epidermal growth factor receptor (EGFR) and anaplastic lymphoma kinase (ALK) wild type (only applicable to patients with non-squamous NSCLC)
Regardless of PD-L1 expression level. However, the number of patients with high level of PD-L1 expression (≥50% PD-L1) will be limited to a maximum of 10 patients
Eastern Cooperative Oncology Group (ECOG, R01-0787) score: 0 to 1
Life expectancy of at least 12 weeks after the start of the treatment according to the Investigator's judgement
Male or female patients. Women of childbearing potential (WOCBP) and men able to father a child must be ready and able to use highly effective methods of birth control (that result in a low failure rate of less than 1% per year when used consistently and correctly) during trial participation and for at least 6 months after the last administration of trial medication. A list of contraception methods meeting these criteria is provided in the patient information.
Exclusion Criteria:
Major surgery (major according to the Investigator's assessment) performed within 12 weeks prior to first trial treatment or planned within 12 months after screening, e.g., hip replacement
Patients who must or wish to continue the intake of restricted medications (see Section 4.2.2.2) or any drug considered likely to interfere with the safe conduct of the trial
Previous enrolment in this trial
Any investigational or anti-tumour treatment, except BI 754091, within 4 weeks or within 5 half-life periods (whichever is shorter) prior to the initiation of trial treatment.
Any unresolved toxicities from prior therapy greater than CTCAE Grade 1 at the time of starting study treatment with the exception of alopecia and Grade 2 neuropathy due to prior platinum-based therapy
Prior treatment with anti-Lymphocyte-activation gene 3 (LAG-3) agents
Patients with NSCLC that has EGFR mutations or ALK rearrangements (only applicable to patients with non-squamous NSCLC).
Presence of other active invasive cancers other than the one treated in this trial within 5 years prior to screening, with the exception of appropriately treated basal-cell carcinoma of the skin, in situ carcinoma of the uterine cervix, or other local tumours considered cured by local treatment
Untreated brain metastasis(es) that may be considered active. Patients with previously treated brain metastases may participate provided they are stable (i.e., without evidence of PD by imaging for at least 4 weeks prior to the first dose of trial treatment, and any neurologic symptoms have returned to baseline), and there is no evidence of new or enlarging brain metastases.
Inadequate organ function or bone marrow reserve as demonstrated by the laboratory values presented in Table 3.3.3: 1.
Any of the following cardiac criteria:
Mean resting corrected QT interval (QTc) >470 msec
Any clinically important abnormalities (as assessed by the Investigator) in rhythm, conduction, or morphology of resting ECGs, e.g., complete left bundle branch block, third degree heart block
Any factors that increase the risk of QTc prolongation or risk of arrhythmic events such as heart failure, hypokalaemia, congenital long QT syndrome, family history of long QT syndrome or unexplained sudden death under 40 years-of-age, or any concomitant medication known to prolong the QT interval
Patients with an ejection fraction (EF) <55% or the lower limit of normal of the institutional standard will be excluded. Only in cases where the Investigator (or the treating physician or both) suspects cardiac disease with negative effect on the EF, will the EF be measured during screening using an appropriate method according to local standards to confirm eligibility (e.g., echocardiogram, multi-gated acquisition scan). A historic measurement of EF no older than 6 months prior to first administration of study drug can be accepted provided that there is clinical evidence that the EF value has not worsened since this measurement in the opinion of the Investigator or of the treating physician or both.
History of pneumonitis within the last 5 years
History of severe hypersensitivity reactions to other mAbs
Immunosuppressive corticosteroid doses (>10 mg prednisone daily or equivalent) within 4 weeks prior to the first dose of study treatment.
Active autoimmune disease or a documented history of autoimmune disease, except vitiligo or resolved childhood asthma/atopy
Active infection requiring systemic treatment (antibacterial, antiviral, or antifungal therapy) at start of treatment in this trial
Known history of human immunodeficiency virus infection or an active hepatitis B or C virus infection
Interstitial lung disease
Chronic alcohol or drug abuse or any condition that, in the Investigator's opinion, makes him/her an unreliable trial subject, unlikely to complete the trial, or unable to comply with the protocol procedures.
Zettl M, Wurm M, Schaaf O, Mostbock S, Tirapu I, Apfler I, Lorenz IC, Frego L, Kenny C, Thibodeau M, Oquendo Cifuentes E, Reschke M, Moll J, Kraut N, Vogt A, Sedgwick JD, Waizenegger IC. Combination of two novel blocking antibodies, anti-PD-1 antibody ezabenlimab (BI 754091) and anti-LAG-3 antibody BI 754111, leads to increased immune cell responses. Oncoimmunology. 2022 Jun 16;11(1):2080328. doi: 10.1080/2162402X.2022.2080328. eCollection 2022.
Clinical studies sponsored by Boehringer Ingelheim, phases I to IV, interventional and non-interventional, are in scope for sharing of the raw clinical study data and clinical study documents, except for the following exclusions:
1. studies in products where Boehringer Ingelheim is not the license holder; 2. studies regarding pharmaceutical formulations and associated analytical methods, and studies pertinent to pharmacokinetics using human biomaterials; 3. studies conducted in a single center or targeting rare diseases (because of limitations with anonymization). For more details refer to: https://www.mystudywindow.com/msw/datasharing
Types
Not provided
Time Frame
Not provided
Access Criteria
Not provided
URL
Not provided
Results Section
Participant Flow Module
Pre-assignment Details
All subjects were screened for eligibility prior to participation in the trial. Subjects attended a specialist site which ensured that they (the subjects) strictly met all inclusion and none of the exclusion criteria. Subjects were not to be allocated to a treatment group if any of the entry criteria were violated.
Recruitment Details
This was an an open label, Phase I dose-finding study in patients with advanced solid cancers followed by expansion cohorts at the selected dose of the combination in patients with non-small cell lung cancer and other solid tumors.
800 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Drug: Ezabenlimab
Drug: BI 754111
Dose-Expansion Cohort G
Experimental
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
Drug: Ezabenlimab
Drug: BI 754111
Dose-Expansion Cohort H
Experimental
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
Drug: Ezabenlimab
Drug: BI 754111
Dose-Expansion Cohort I
Experimental
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
Drug: Ezabenlimab
Drug: BI 754111
Dose-Expansion Cohort J
Experimental
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (≥50% PD-L1) were enrolled.
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 1286 days.
Dose Escalation: Number of Patients Experiencing DLTs
Dose escalation: Number of patients experiencing DLTs from start of treatment until end of treatment (in all cycles).
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 1286 days.
Dose Expansion: Duration of Response
Duration of response is measured from the time measurements criteria are met for CR/PR (whichever is first recorded) until the first date that recurrent or progressive disease (PD) is objectively documented (taking as reference for PD the smallest measurements recorded since the treatment started).
From the date of objective response until first date that recurrent or PD has been documented, up to 100 weeks.
Dose Expansion: Percentage of Patients With Disease Control
Dose expansion: Percentage of patients with disease control (CR, PR, or stable disease (SD) according to RECIST Version 1.1) as assessed by the Investigator.
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 818 days.
Dose Expansion: Progression-free Survival (PFS)
Dose expansion: Progression-free survival (PFS) is defined as time from first drug intake until disease progression or death from any cause, whichever occurs earlier. The date of progression will be based on the Investigator assessment according to RECIST 1.1.
For patients with 'event' as an outcome for PFS:
• PFS [days] = date of outcome - date of start of treatment + 1
For patients with 'censored' as an outcome for PFS:
• PFS (censored) [days] = date of outcome - date of start of treatment + 1
Days were converted into months for reporting.
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 818 days.
Dose Expansion: Number of Patients Experiencing DLTs
Dose expansion: Number of patients experiencing DLTs from start of treatment until end of treatment.
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 818 days.
Dose Escalation: AUC0-504: Area Under the Concentration-time Curve of Ezabenlimab in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: AUC0-504: area under the concentration-time curve of ezabenlimab in plasma over the time interval from 0 to 504 hours.
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the first treatment cycle.
Dose Escalation: AUC0-504 Steady State: Area Under the Concentration-time Curve of Ezabenlimab in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: AUC0-504 steady state: area under the concentration-time curve of ezabenlimab in plasma over the time interval from 0 to 504 hours at steady state.
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the fourth treatment cycle.
Dose Escalation: AUC0-504: Area Under the Concentration-time Curve of BI 754111 in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: AUC0-504: area under the concentration-time curve of BI 754111 in plasma over the time interval from 0 to 504 hours.
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the first treatment cycle.
Dose Escalation: AUC0-504 Steady State: Area Under the Concentration-time Curve of BI 754111 in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: AUC0-504 steady state: area under the concentration-time curve of BI 754111 in plasma over the time interval from 0 to 504 hours at steady state.
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the fourth treatment cycle.
Dose Escalation: Cmax: Maximum Measured Concentration of Ezabenlimab in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: Cmax: maximum measured concentration of ezabenlimab in plasma over the time interval from 0 to 504 hours.
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the first treatment cycle.
Dose Escalation: Cmax Steady State: Maximum Measured Concentration of Ezabenlimab in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: Cmax steady state: maximum measured concentration of ezabenlimab in plasma over the time interval from 0 to 504 hours at steady state.
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the fourth treatment cycle.
Dose Escalation: Cmax: Maximum Measured Concentration of BI 754111 in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: Cmax: maximum measured concentration of BI 754111 in plasma over the time interval from 0 to 504 hours.
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the first treatment cycle.
Dose Escalation: Cmax Steady State: Maximum Measured Concentration of BI 754111 in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: Cmax steady state: maximum measured concentration of BI 754111 in plasma over the time interval from 0 to 504 hours at steady state.
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the fourth treatment cycle.
Sarasota
Florida
34232
United States
John Theurer Cancer Center
Hackensack
New Jersey
07601
United States
Stephenson Cancer Center
Oklahoma City
Oklahoma
73104
United States
Tennessee Oncology, PLLC
Nashville
Tennessee
37203
United States
Froedtert and The Medical College of Wisconsin
Milwaukee
Wisconsin
53226
United States
Cross Cancer Institute (University of Alberta)
Edmonton
Alberta
T6G 1Z2
Canada
Princess Margaret Cancer Centre
Toronto
Ontario
M5G 1Z9
Canada
BioVirtus Research Site Sp. z o.o.
Józefów
05-410
Poland
Oncology Center-Maria Sklodowska-Curie Institute
Warsaw
02-781
Poland
Hospital Universitari Dexeus
Barcelona
08028
Spain
Hospital General Universitario Gregorio Marañón
Madrid
28007
Spain
Hospital Universitario HM Sanchinarro
Madrid
28050
Spain
Hospital Politècnic La Fe
Valencia
46026
Spain
Sarah Cannon Research Institute
London
W1G 6AD
United Kingdom
20 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
800 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
FG007
Dose-Expansion Cohort G
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
FG008
Dose-Expansion Cohort H
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
FG009
Dose-Expansion Cohort I
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
FG010
Dose-Expansion Cohort J
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (≥50% PD-L1) were enrolled.
FG0004 subjects
FG0019 subjects
FG0029 subjects
FG0039 subjects
FG0049 subjects
FG0059 subjects
FG0066 subjects
FG00721 subjects
FG00840 subjects
FG00939 subjects
FG01017 subjects
COMPLETED
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0030 subjects
FG0040 subjects
FG0050 subjects
FG0060 subjects
FG0070 subjects
FG0080 subjects
FG0090 subjects
FG0100 subjects
NOT COMPLETED
FG0004 subjects
FG0019 subjects
FG0029 subjects
FG0039 subjects
FG0049 subjects
FG0059 subjects
FG0066 subjects
FG00721 subjects
FG00840 subjects
FG00939 subjects
FG01017 subjects
Type
Comment
Reasons
Other than listed
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0030 subjects
FG0040 subjects
FG0050 subjects
FG0060 subjects
FG0070 subjects
FG0080 subjects
FG0091 subjects
FG0101 subjects
Subject decision
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0030 subjects
FG004
Physician Decision
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0031 subjects
FG004
Non-compliant with study drug
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0031 subjects
FG004
Death
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0030 subjects
FG004
Adverse Event
FG0000 subjects
FG0011 subjects
FG0021 subjects
FG0032 subjects
FG004
Progressive disease
FG0004 subjects
FG0018 subjects
FG0028 subjects
FG0035 subjects
FG004
Currently on treatment
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0030 subjects
FG004
The Treated Set (TS) included all patients who received at least 1 dose of BI 754111 or ezabenlimab.
800 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
BG007
Dose-Expansion Cohort G
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
BG008
Dose-Expansion Cohort H
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
BG009
Dose-Expansion Cohort I
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
BG010
Dose-Expansion Cohort J
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (≥50% PD-L1) were enrolled.
BG011
Total
Total of all reporting groups
Denominators
Units
Counts
Participants
BG0004
BG0019
BG0029
BG0039
BG0049
BG0059
BG0066
BG00721
BG00840
BG00939
BG01017
BG011172
Baseline Measures
Title
Description
Population Description
Parameter Type
Dispersion Type
Unit of Measure
Calculate Percentage
Denominator Units Selected
Denominators
Classes
Age, Continuous
Mean
Standard Deviation
years
Title
Denominators
Categories
Title
Measurements
BG00066.5± 9.7
BG00162.3± 10.8
BG00261.8± 5.5
BG003
Sex: Female, Male
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
Female
BG0001
BG0018
BG002
Ethnicity (NIH/OMB)
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
Hispanic or Latino
BG0000
BG0010
BG002
Race (NIH/OMB)
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
American Indian or Alaska Native
BG0000
BG0010
BG002
Type
Title
Description
Population Description
Reporting Status
Anticipated Posting Date
Parameter Type
Dispersion Type
Unit of Measure
Calculate Percentage
Time Frame
Units Analyzed
Denominator Units Selected
Arm/Group Information
Denominators
Classes
Analyses
Primary
Dose Escalation: Maximum-tolerated Dose (MTD) of the BI 754111 Plus Ezabenlimab Combination
The MTD is defined as the highest dose with less than 25% risk of the true Dose-limiting toxicity (DLT) rate being above 33%. DLTs include:
Haematologic toxicities:
Any Grade 5 toxicity
Neutropenia ≥ Grade 4 for >5 days
Any duration febrile neutropenia
Grade 4 thrombocytopenia or Grade 3 with bleeding/platelet transfusion need
Unexplained Grade 4 anaemia.
Non-haematological toxicities:
Aspartate aminotransferase (AST) or Alanine aminotransferase (ALT) >3x Upper limit of normal (ULN) and total bilirubin >2x ULN without cholestasis signs
≥Grade 4 AST or ALT of any duration
Any ≥Grade 3 non-haematologic toxicity with exceptions
Any Grade 4 or 5 adverse event (AE)
Any Grade 2 pneumonitis
Any Grade 2 uveitis, eye pain, or blurred vision not improving to Grade 1 within 2 weeks or requiring systemic treatment
Any ≥ Grade 2 toxicity causing inability to administer BI 754091 on Cycle 2 Day 1.
The MTD evaluation set included all patients in the dose escalation cohort who received BI 754111 or ezabenlimab, and who were not replaced within the MTD evaluation period (First treatment cycle, the first 21 days following the start of trial medication).
Posted
Number
Milligram
First treatment cycle, the first 21 days following the start of trial medication.
ID
Title
Description
OG000
Dose Escalation Cohort: BI 754111 + Ezabenlimab
Comprises all dose cohorts during the dose escalation phase. BI 754111 and ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Units
Counts
Participants
OG00055
Title
Denominators
Categories
Title
Measurements
OG000NAThere were no dose-limiting toxicities experienced by any dose escalation cohort patient during the MTD evaluation period, thus MTD was not reached.
Primary
Dose Escalation: Number of Patients Experiencing DLTs During the Combination MTD Evaluation Period
Number of patients experiencing DLTs during the combination MTD evaluation period (first cycle of BI 754111 plus ezabenlimab combination therapy) in patients with solid tumours.
The MTD evaluation set included all patients in the dose escalation cohort who received BI 754111 or ezabenlimab, and who were not replaced within the MTD evaluation period (First treatment cycle, the first 21 days following the start of trial medication).
Posted
Count of Participants
Participants
First treatment cycle, the first 21 days following the start of trial medication.
80 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Primary
Dose Expansion: Number of Patients With Objective Response (OR) - Confirmed Complete Response (CR) and Partial Response (PR)
Dose expansion: Number of patients with objective response (OR) - confirmed complete response (CR) and partial response (PR) according to Response Evaluation Criteria in Solid Tumours (RECIST) Version 1.1 as assessed by the Investigator during the entire treatment.
Complete Response (CR): Disappearance of all target lesions. Any pathological lymph nodes (whether target or non-target) must have reduction in short axis to <10 millimeter.
Partial Response (PR): At least a 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters.
The Treated Set (TS) included all patients in the dose expansion cohort who received at least 1 dose of BI 754111 or ezabenlimab and had a post baseline measurement.
Posted
Count of Participants
Participants
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 818 days.
ID
Title
Description
OG000
Dose-Expansion Cohort G
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
OG001
Dose-Expansion Cohort H
Secondary
Dose Escalation: Number of Patients With Objective Response (OR) - Confirmed Complete Response (CR) and Partial Response (PR)
Dose escalation: Number of patients with objective response (OR) - confirmed complete response (CR) and partial response (PR) according to RECIST Version 1.1 as assessed by the Investigator during the entire treatment.
Complete Response (CR): Disappearance of all target lesions. Any pathological lymph nodes (whether target or non-target) must have reduction in short axis to <10 millimeter.
Partial Response (PR): At least a 30% decrease in the sum of diameters of target lesions, taking as reference the baseline sum diameters.
The Treated Set (TS) included all patients in the dose escalation cohort who received at least 1 dose of BI 754111 or ezabenlimab and had a post baseline measurement.
Posted
Count of Participants
Participants
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 1286 days.
20 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Secondary
Dose Escalation: Number of Patients Experiencing DLTs
Dose escalation: Number of patients experiencing DLTs from start of treatment until end of treatment (in all cycles).
The Treated Set (TS) included all patients in the dose escalation cohort who received at least 1 dose of BI 754111 or ezabenlimab and had a post baseline measurement.
Posted
Count of Participants
Participants
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 1286 days.
80 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Secondary
Dose Expansion: Duration of Response
Duration of response is measured from the time measurements criteria are met for CR/PR (whichever is first recorded) until the first date that recurrent or progressive disease (PD) is objectively documented (taking as reference for PD the smallest measurements recorded since the treatment started).
The Treated Set (TS) included all patients in the dose expansion cohort who received at least 1 dose of BI 754111 or ezabenlimab and had a post baseline measurement and had an objective response.
Posted
Median
Standard Deviation
Weeks
From the date of objective response until first date that recurrent or PD has been documented, up to 100 weeks.
ID
Title
Description
OG000
Dose-Expansion Cohort G
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
OG001
Dose-Expansion Cohort H
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
OG002
Secondary
Dose Expansion: Percentage of Patients With Disease Control
Dose expansion: Percentage of patients with disease control (CR, PR, or stable disease (SD) according to RECIST Version 1.1) as assessed by the Investigator.
The Treated Set (TS) included all patients in the dose expansion cohort who received at least 1 dose of BI 754111 or ezabenlimab and had a post baseline measurement.
Posted
Number
95% Confidence Interval
Percentage of participants
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 818 days.
ID
Title
Description
OG000
Dose-Expansion Cohort G
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
OG001
Dose-Expansion Cohort H
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
OG002
Dose-Expansion Cohort I
Secondary
Dose Expansion: Progression-free Survival (PFS)
Dose expansion: Progression-free survival (PFS) is defined as time from first drug intake until disease progression or death from any cause, whichever occurs earlier. The date of progression will be based on the Investigator assessment according to RECIST 1.1.
For patients with 'event' as an outcome for PFS:
• PFS [days] = date of outcome - date of start of treatment + 1
For patients with 'censored' as an outcome for PFS:
• PFS (censored) [days] = date of outcome - date of start of treatment + 1
Days were converted into months for reporting.
The Treated Set (TS) included all patients in the dose expansion cohort who received at least 1 dose of BI 754111 or ezabenlimab and had a post baseline measurement.
Posted
Median
Inter-Quartile Range
Months
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 818 days.
ID
Title
Description
OG000
Dose-Expansion Cohort G
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
OG001
Dose-Expansion Cohort H
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
Secondary
Dose Expansion: Number of Patients Experiencing DLTs
Dose expansion: Number of patients experiencing DLTs from start of treatment until end of treatment.
The Treated Set (TS) included all patients in the dose expansion cohort who received at least 1 dose of BI 754111 or ezabenlimab and had a post baseline measurement.
Posted
Count of Participants
Participants
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 818 days.
ID
Title
Description
OG000
Dose-Expansion Cohort G
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
OG001
Dose-Expansion Cohort H
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
OG002
Dose-Expansion Cohort I
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
Secondary
Dose Escalation: AUC0-504: Area Under the Concentration-time Curve of Ezabenlimab in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: AUC0-504: area under the concentration-time curve of ezabenlimab in plasma over the time interval from 0 to 504 hours.
All patients in the TS who provided at least one evaluable observation for at least one Pharmacokinetic (PK) endpoint and no PK relevant protocol deviations. Only patients in the dose escalation cohort with non-missing data were included.
Posted
Geometric Mean
Geometric Coefficient of Variation
microgram*hours/milliliter
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the first treatment cycle.
80 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Secondary
Dose Escalation: AUC0-504 Steady State: Area Under the Concentration-time Curve of Ezabenlimab in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: AUC0-504 steady state: area under the concentration-time curve of ezabenlimab in plasma over the time interval from 0 to 504 hours at steady state.
All patients in the TS who provided at least one evaluable observation for at least one PK endpoint and no PK relevant protocol deviations. Only patients in the dose escalation cohort with non-missing data were included.
Posted
Geometric Mean
Geometric Coefficient of Variation
microgram*hours/milliliter
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the fourth treatment cycle.
Dose Escalation: AUC0-504: Area Under the Concentration-time Curve of BI 754111 in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: AUC0-504: area under the concentration-time curve of BI 754111 in plasma over the time interval from 0 to 504 hours.
All patients in the TS who provided at least one evaluable observation for at least one PK endpoint and no PK relevant protocol deviations. Only patients in the dose escalation cohort with non-missing data who had enough data to calculate the endpoint were included.
Posted
Geometric Mean
Geometric Coefficient of Variation
microgram*hours/milliliter
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the first treatment cycle.
Dose Escalation: AUC0-504 Steady State: Area Under the Concentration-time Curve of BI 754111 in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: AUC0-504 steady state: area under the concentration-time curve of BI 754111 in plasma over the time interval from 0 to 504 hours at steady state.
All patients in the TS who provided at least one evaluable observation for at least one PK endpoint and no PK relevant protocol deviations. Only patients in the dose escalation cohort with non-missing data who had enough data to calculate the endpoint were included.
Posted
Geometric Mean
Geometric Coefficient of Variation
microgram*hours/milliliter
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the fourth treatment cycle.
Dose Escalation: Cmax: Maximum Measured Concentration of Ezabenlimab in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: Cmax: maximum measured concentration of ezabenlimab in plasma over the time interval from 0 to 504 hours.
All patients in the TS who provided at least one evaluable observation for at least one PK endpoint and no PK relevant protocol deviations. Only patients in the dose escalation cohort with non-missing data were included.
Posted
Geometric Mean
Geometric Coefficient of Variation
microgram/milliliter
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the first treatment cycle.
80 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Secondary
Dose Escalation: Cmax Steady State: Maximum Measured Concentration of Ezabenlimab in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: Cmax steady state: maximum measured concentration of ezabenlimab in plasma over the time interval from 0 to 504 hours at steady state.
All patients in the TS who provided at least one evaluable observation for at least one PK endpoint and no PK relevant protocol deviations. Only patients in the dose escalation cohort with non-missing data were included.
Posted
Geometric Mean
Geometric Coefficient of Variation
microgram/milliliter
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the fourth treatment cycle.
80 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Secondary
Dose Escalation: Cmax: Maximum Measured Concentration of BI 754111 in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: Cmax: maximum measured concentration of BI 754111 in plasma over the time interval from 0 to 504 hours.
All patients in the TS who provided at least one evaluable observation for at least one PK endpoint and no PK relevant protocol deviations. Only patients in the dose escalation cohort with non-missing data were included.
Posted
Geometric Mean
Geometric Coefficient of Variation
microgram/milliliter
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the first treatment cycle.
80 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Secondary
Dose Escalation: Cmax Steady State: Maximum Measured Concentration of BI 754111 in Plasma Over the Time Interval From 0 to 504 Hours
Dose escalation: Cmax steady state: maximum measured concentration of BI 754111 in plasma over the time interval from 0 to 504 hours at steady state.
All patients in the TS who provided at least one evaluable observation for at least one PK endpoint and no PK relevant protocol deviations. Only patients in the dose escalation cohort with non-missing data were included.
Posted
Geometric Mean
Geometric Coefficient of Variation
microgram/milliliter
Within 1 hour before and 1, 4, 7, 24, 72, 168, 336 and 504 hours following the start of infusion in the fourth treatment cycle.
80 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Time Frame
From the date of the first administration of trial treatment until the date of the last administration of trial treatment + 30 days (residual effect period), up to 1286 days.
Description
The Treated Set (TS) included all patients who received at least 1 dose of BI 754111 or ezabenlimab.
800 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
0
6
2
6
6
6
EG007
Dose-Expansion Cohort G
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with 2nd and 3rd line Non-small cell lung cancer (NSCLC) who progressed on anti-programmed cell death 1 (PD-1) or anti-programmed cell death ligand 1 (PD-L1) treatment.
16
21
8
21
18
21
EG008
Dose-Expansion Cohort H
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
27
40
16
40
39
40
EG009
Dose-Expansion Cohort I
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
25
39
21
39
36
39
EG010
Dose-Expansion Cohort J
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (=50% PD-L1) were enrolled.
11
17
8
17
16
17
Serious Adverse Events
Term
Organ System
Source Vocabulary
Assessment Type
Notes
Statistical Information
Anaemia
Blood and lymphatic system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG0030 affected9 at risk
EG0040 affected9 at risk
EG0051 affected9 at risk
EG0060 affected6 at risk
EG0070 affected21 at risk
EG0080 affected40 at risk
EG0090 affected39 at risk
EG0100 affected17 at risk
Acute left ventricular failure
Cardiac disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Adrenal insufficiency
Endocrine disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Abdominal pain
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Ascites
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Colitis
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Constipation
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Diarrhoea
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Enterocutaneous fistula
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Gastric perforation
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Gastric ulcer haemorrhage
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Haematochezia
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Ileus
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pancreatitis
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Proctalgia
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Small intestinal obstruction
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Upper gastrointestinal haemorrhage
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Vomiting
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Asthenia
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Influenza like illness
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Mucosal inflammation
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pyrexia
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Autoimmune hepatitis
Hepatobiliary disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Liver injury
Hepatobiliary disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Portal vein thrombosis
Hepatobiliary disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Contrast media reaction
Immune system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Bacteraemia
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Cellulitis
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Cytomegalovirus colitis
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Encephalitis
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Klebsiella sepsis
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Meningitis aseptic
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Perirectal abscess
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pneumonia
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Postoperative wound infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pulmonary sepsis
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Respiratory tract infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Sepsis
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Septic shock
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Urinary tract infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Infusion related reaction
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Radiation necrosis
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Thermal burn
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Clostridium test positive
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Diabetic ketoacidosis
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hyperglycaemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Arthralgia
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Back pain
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pain in extremity
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Soft tissue haemorrhage
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Tumour pain
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Encephalopathy
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Guillain-Barre syndrome
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Neuropathy peripheral
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Seizure
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Confusional state
Psychiatric disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Haematuria
Renal and urinary disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Chronic obstructive pulmonary disease
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Dyspnoea
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pleural effusion
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pneumonitis
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pneumothorax
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pulmonary embolism
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Respiratory failure
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Rash macular
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Deep vein thrombosis
Vascular disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Embolism
Vascular disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Other Adverse Events
Term
Organ System
Source Vocabulary
Assessment Type
Notes
Statistical Information
Anaemia
Blood and lymphatic system disorders
MedDRA 26.0
Systematic Assessment
EG0002 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG0032 affected9 at risk
EG0042 affected9 at risk
EG0051 affected9 at risk
EG0060 affected6 at risk
EG0071 affected21 at risk
EG0083 affected40 at risk
EG0094 affected39 at risk
EG0102 affected17 at risk
Iron deficiency anaemia
Blood and lymphatic system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Leukocytosis
Blood and lymphatic system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Lymphopenia
Blood and lymphatic system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Neutrophilia
Blood and lymphatic system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Atrial fibrillation
Cardiac disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Atrial flutter
Cardiac disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Sinus tachycardia
Cardiac disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Ear congestion
Ear and labyrinth disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Middle ear effusion
Ear and labyrinth disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Tinnitus
Ear and labyrinth disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Goitre
Endocrine disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hyperthyroidism
Endocrine disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Hypothyroidism
Endocrine disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0021 affected9 at risk
EG003
Thyroiditis
Endocrine disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Diplopia
Eye disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Dry eye
Eye disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Eyelid pain
Eye disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Vision blurred
Eye disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Visual impairment
Eye disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Abdominal distension
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0012 affected9 at risk
EG0020 affected9 at risk
EG003
Abdominal pain
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0021 affected9 at risk
EG003
Abdominal pain upper
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Colitis
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Constipation
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0021 affected9 at risk
EG003
Dental caries
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Diarrhoea
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0022 affected9 at risk
EG003
Dry mouth
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Dyspepsia
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Dysphagia
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Flatulence
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Gastrooesophageal reflux disease
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Haematochezia
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Immune-mediated enterocolitis
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Nausea
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0003 affected4 at risk
EG0012 affected9 at risk
EG0021 affected9 at risk
EG003
Proctalgia
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Rectal haemorrhage
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Vomiting
Gastrointestinal disorders
MedDRA 26.0
Systematic Assessment
EG0002 affected4 at risk
EG0012 affected9 at risk
EG0021 affected9 at risk
EG003
Asthenia
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Axillary pain
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Catheter site pain
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Catheter site rash
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Chest discomfort
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Chest pain
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0021 affected9 at risk
EG003
Chills
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Fatigue
General disorders
MedDRA 26.0
Systematic Assessment
EG0003 affected4 at risk
EG0012 affected9 at risk
EG0022 affected9 at risk
EG003
Feeling cold
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Feeling hot
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Generalised oedema
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Influenza like illness
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Malaise
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Mucosal inflammation
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Non-cardiac chest pain
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Oedema
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Oedema peripheral
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0021 affected9 at risk
EG003
Pain
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Peripheral swelling
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pyrexia
General disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0012 affected9 at risk
EG0022 affected9 at risk
EG003
Seasonal allergy
Immune system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Bacteraemia
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
COVID-19
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Candida infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Clostridium difficile infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Herpes zoster
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Influenza
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Nasopharyngitis
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Oral herpes
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Otitis media
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pneumonia
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Sinusitis
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Skin infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Upper respiratory tract infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Urinary tract infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0013 affected9 at risk
EG0021 affected9 at risk
EG003
Viral infection
Infections and infestations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Contusion
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Fall
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Fracture
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Infusion related reaction
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0012 affected9 at risk
EG0020 affected9 at risk
EG003
Rib fracture
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Vascular access complication
Injury, poisoning and procedural complications
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Alanine aminotransferase increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0022 affected9 at risk
EG003
Amylase increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Aspartate aminotransferase increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0022 affected9 at risk
EG003
Blood alkaline phosphatase increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Blood bilirubin increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Blood creatine phosphokinase increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Blood creatinine increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Blood glucose increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Blood potassium increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Blood thyroid stimulating hormone increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Lipase increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Liver function test increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Serum ferritin decreased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Troponin increased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Weight decreased
Investigations
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0021 affected9 at risk
EG003
Decreased appetite
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0013 affected9 at risk
EG0021 affected9 at risk
EG003
Dehydration
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Glucose tolerance impaired
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0021 affected9 at risk
EG003
Hyperglycaemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hyperkalaemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypoalbuminaemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypocalcaemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypochloraemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypoglycaemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypokalaemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0012 affected9 at risk
EG0022 affected9 at risk
EG003
Hypomagnesaemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hyponatraemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypophosphataemia
Metabolism and nutrition disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Arthralgia
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected9 at risk
EG0022 affected9 at risk
EG003
Arthritis
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Autoimmune arthritis
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Back pain
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Flank pain
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Muscle spasms
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Muscular weakness
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Musculoskeletal chest pain
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Musculoskeletal pain
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Myalgia
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Neck pain
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Pain in extremity
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Polyarthritis
Musculoskeletal and connective tissue disorders
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Aphasia
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Ataxia
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Dizziness
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Dysgeusia
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Headache
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Hypoaesthesia
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hyposmia
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Neurotoxicity
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Paraesthesia
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Post herpetic neuralgia
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Presyncope
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Somnolence
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Syncope
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Taste disorder
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Tremor
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Trigeminal neuralgia
Nervous system disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Device malfunction
Product issues
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Agitation
Psychiatric disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Anxiety
Psychiatric disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Confusional state
Psychiatric disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Depression
Psychiatric disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Insomnia
Psychiatric disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Chronic kidney disease
Renal and urinary disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Dysuria
Renal and urinary disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Pollakiuria
Renal and urinary disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Urinary retention
Renal and urinary disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pelvic pain
Reproductive system and breast disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Vaginal discharge
Reproductive system and breast disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Chronic obstructive pulmonary disease
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Cough
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0002 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Dysphonia
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Dyspnoea
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0013 affected9 at risk
EG0021 affected9 at risk
EG003
Dyspnoea exertional
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Haemoptysis
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hiccups
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypoxia
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Laryngeal inflammation
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Lower respiratory tract congestion
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Nasal congestion
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Oropharyngeal pain
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Pleural effusion
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pneumonitis
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Productive cough
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pulmonary pain
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Rhinitis allergic
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Sinus congestion
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Wheezing
Respiratory, thoracic and mediastinal disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Alopecia
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Dermatitis acneiform
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Dry skin
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hyperhidrosis
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Lichenoid keratosis
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Pruritus
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0022 affected9 at risk
EG003
Rash
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Rash macular
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Rash maculo-papular
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Skin disorder
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected9 at risk
EG0020 affected9 at risk
EG003
Urticaria
Skin and subcutaneous tissue disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypertension
Vascular disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0020 affected9 at risk
EG003
Hypotension
Vascular disorders
MedDRA 26.0
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected9 at risk
EG0021 affected9 at risk
EG003
Certain Agreements
Are all PI(s) employees of the sponsor?
No
Restriction Type
OTHER
Results Disclosure Restriction on PI(s)?
Yes
Other Details
Boehringer Ingelheim (BI) acknowledges that investigators have the right to publish the study results. Investigators shall provide BI with a copy of any publication or presentation for review prior to any submission. Such review will be done with regard to proprietary information, information related to patentable inventions, medical, scientific, and statistical accuracy within 60 days. BI may request a delay of the publication in order to protect BI's intellectual property rights.
800 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Units
Counts
Participants
OG0004
OG0019
OG0029
OG0039
OG0049
OG0059
OG0066
Title
Denominators
Categories
Title
Measurements
OG0000
OG0010
OG0020
OG0030
OG0040
OG0050
OG0060
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in ≥2nd line microsatellite stable anti-PD-1 and anti-PD-L1 treatment-naïve metastatic colorectal cancer (mCRC).
OG002
Dose-Expansion Cohort I
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
OG003
Dose-Expansion Cohort J
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (=50% PD-L1) were enrolled.
800 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w).
Units
Counts
Participants
OG0004
OG0019
OG0029
OG0039
OG0049
OG0059
OG0066
Title
Denominators
Categories
Title
Measurements
OG0000
OG0010
OG0020
OG0030
OG0040
OG0051
OG0060
Dose-Expansion Cohort I
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
OG003
Dose-Expansion Cohort J
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (=50% PD-L1) were enrolled.
Units
Counts
Participants
OG0000
OG0013
OG0024
OG0033
Title
Denominators
Categories
Title
Measurements
OG00141.14± 31.74
OG00245.93± 31.37
OG00321.57± 49.22
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
OG003
Dose-Expansion Cohort J
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (=50% PD-L1) were enrolled.
Units
Counts
Participants
OG00018
OG00136
OG00237
OG00315
Title
Denominators
Categories
Title
Measurements
OG00044.4(21.5 to 69.2)
OG00138.9(23.1 to 56.5)
OG00243.2(27.1 to 60.5)
OG00386.7(59.5 to 98.3)
OG002
Dose-Expansion Cohort I
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) in patients with any solid tumour with high tumour mutational burden (TMB) and/or microsatellite instability high (MSI-H) and/or DNA mismatch repair deficient solid tumours who have received 1 prior anti-PD-1 or anti-PD-L1 treatment regimen.
OG003
Dose-Expansion Cohort J
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (=50% PD-L1) were enrolled.
Units
Counts
Participants
OG00021
OG00140
OG00239
OG00317
Title
Denominators
Categories
Title
Measurements
OG0002.3(1.4 to 5.7)
OG0011.4(1.3 to 2.8)
OG0021.5(1.3 to 4.1)
OG0035.5(2.7 to 13.7)
OG003
Dose-Expansion Cohort J
600 milligram (mg) BI 754111 and 240 mg ezabenlimab given as an intravenous infusion on day 1 of 21-day cycles (q3w) patients with 1st line epidermal growth factor receptor (EGFR) wildtype (WT) and anaplastic lymphoma kinase (ALK) wildtype NSCLC. Patients may have any level of PD-L1 expression, but only a maximum of 10 patients with PD-L1 high expression (=50% PD-L1) were enrolled.