A Phase 1b Open-Label Study Investigating the Safety and... | NCT02961881 | Trialant
NCT02961881
Sponsor
Amgen
Status
Completed
Last Update Posted
Feb 2, 2024Actual
Enrollment
35Actual
Phase
Phase 1
Conditions
Non-Hodgkin's Lymphoma
Interventions
blinatumomab
Countries
United States
Australia
France
Germany
Italy
United Kingdom
Protocol Section
Identification Module
NCT ID
NCT02961881
Obsolete or Duplicate NCT IDs
Not provided
Organization Study
20140286
Secondary IDs
ID
Type
Description
Link
2016-002034-76
EudraCT Number
Brief Title
A Phase 1b Open-Label Study Investigating the Safety and Pharmacokinetics of Administration of Subcutaneous Blinatumomab for the Treatment of Relapsed/Refractory Indolent Non-Hodgkin's Lymphoma
Official Title
A Phase 1b Open-Label Study Investigating the Safety and Pharmacokinetics of Administration of Subcutaneous Blinatumomab for the Treatment of Relapsed/Refractory Indolent Non-Hodgkin's Lymphoma
Acronym
Not provided
Organization
AmgenINDUSTRY
Status Module
Record Verification Date
May 2023
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
Sep 18, 2017Actual
Primary Completion Date
Sep 2, 2021Actual
Completion Date
Sep 2, 2021Actual
First Submitted Date
Sep 6, 2016
First Submission Date that Met QC Criteria
Nov 9, 2016
First Posted Date
Nov 11, 2016Estimated
Results Waived
Not provided
Results First Submitted Date
Jul 12, 2022
Results First Submitted that Met QC Criteria
May 30, 2023
Results First Posted Date
Feb 2, 2024Actual
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
May 30, 2023
Last Update Posted Date
Feb 2, 2024Actual
Sponsor/Collaborators Module
Responsible Party, by Official Title
Sponsor
Lead Sponsor
AmgenINDUSTRY
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
Primary Objective:
• To evaluate the safety and tolerability of subcutaneous (SC) blinatumomab dose administrations
Secondary Objectives:
To determine pharmacokinetics (PK) with continuous intravenous (cIV) and SC administrations
To estimate the maximum tolerated dose (MTD) tested for blinatumomab administered subcutaneously
To determine the incidence of anti-blinatumomab antibody formation following SC administration
To evaluate efficacy response following treatment with SC blinatumomab administration
Exploratory Objective:
To determine the pharmacodynamics (PD) time profiles for B-and T-lymphocytes as well as cytokine profiles during SC administration
To evaluate efficacy response following treatment with SC blinatumomab administration using Lugano criteria if positron emission tomography-computed tomography (PET/CT) is used for evaluation
Detailed Description
Not provided
Conditions Module
Conditions
Non-Hodgkin's Lymphoma
Keywords
Not provided
Design Module
Study Type
Interventional
Number of References to an Expanded Access Study
Not provided
Expanded Access Types
Not provided
Patient Registry
Not provided
Target Follow-Up Duration
Not provided
Phases
Phase 1
Interventional Study Design
Allocation
Biospecimen
No data available
No data is available for this block.
Enrollment
35Actual
Arms/Interventions Module
Arm Groups
Label
Type
Description
Intervention Names
blinatumomab
Experimental
Drug: blinatumomab
Interventions
Name
Type
Description
Arm Group Labels
Other Names
blinatumomab
Drug
Blinatumomab used as both continuous IV infusion and subcutaneous injection
blinatumomab
Outcomes Module
Primary Outcomes
Measure
Description
Time Frame
Number of Participants With Dose Limiting-Toxicities (DLTs) After SC Administration
The occurrence of any of the following toxicities during the DLT evaluation period was considered a DLT, if judged by the investigator to be related to the administration of blinatumomab:
Death
Any toxicity, regardless of grade, that lead to a participant's removal from the study by the investigator and/or sponsor
Persistent Common Terminology Criteria for Adverse Events (CTCAE) grade >/= 2 non-hematologic adverse events (AEs) that were deemed intolerable by the participant or the treating physician and that did not respond to appropriate medical management within 5 days and lead to treatment discontinuation
Recurrent grade 2 seizures
All grade 3 and 4 AEs and laboratory abnormalities, which occurred during the SC administration portion of the treatment period with exceptions noted in protocol section 6.2.1.2.3.
Day 1 to Day 7 of Week 4
Number of Participants With DLTs CTCAE Grade ≥ 3 After SC Administration
All toxicities were graded using the CTCAE version 4.0: Grade 1 = mild; Grade 2 = moderate; Grade 3 = severe; Grade 4 = life-threatening; Grade 5 = fatal.
Day 1 to Day 7 of Week 4
Number of Participants With Treatment-emergent Adverse Events (TEAEs) After SC Administration
An AE was defined as any untoward medical occurrence in a clinical study participant. The AE did not necessarily have a causal relationship with study treatment. The definition of AEs included worsening of a pre-existing medical condition.
TEAEs included AEs starting on or after first dose of investigational product and up to the end of study date. All AEs were graded using the CTCAE version 4.0: Grade 1 = mild; Grade 2 = moderate; Grade 3 = severe; Grade 4 = life-threatening; Grade 5 = fatal.
Day 1 to end of study (approximately 17 weeks)
Secondary Outcomes
Measure
Description
Time Frame
Steady State Serum Concentration (Css) of Blinatumomab After cIV Administration
Summarized as the observed concentrations collected after 5 half-lives after the start of the IV infusion of each dose (i.e., 9, 28 and 112 μg/day).
Once at any timepoint during Day 2 of Weeks 1, 2, 3, 5 and 6
Systemic Clearance (CL) of Blinatumomab After cIV Administration
Other Outcomes
Not provided
Eligibility Module
Eligibility Criteria
Inclusion Criteria:
Subject or subject's legally acceptable representative has provided informed consent.
Age greater than or equal to 18 years old at the time of informed consent
Subjects must have a histologically determined B cell NHL subtype as defined in the bullets below.
In addition, they must have disease that is primary refractory after initial therapy or have relapsed disease.
Follicular Lymphoma I, II, IIIA
Marginal zone lymphoma (extranodal, nodal or splenic). Subjects with gastric mucosa-
associated lymphoid tissue must have progressed after Helicobacter pylori therapy and
radiation. Subjects with splenic marginal zone lymphoma must have prior splenectomy.
Lymphoplasmocytic lymphoma
Mantle cell lymphoma ([MCL] with the exception of aggressive MCL, defined as Ki67 > 30%,
or blastoid histology)
Small lymphocytic lymphoma
• Subjects without standard therapy alternatives, or contraindicated for standard therapy by investigator, or subjects unwilling to receive standard therapy. Disease status must be 1 of the following:
Primary refractory (at least 1 prior line of therapy)
Relapsed within 1 year of first response
Responded to initial therapy for ≥ 1 year and relapsed after 2 or more lines of therapy, including an anti-CD20 monoclonal antibody
Measurable disease that has not been previously irradiated on positron emission tomography- computed tomography (PET-CT), or computed tomography (CT), of at least 1.5 cm within the last 21 days before the start of IP treatment.
Eastern Cooperative Oncology Group (ECOG) performance status less than or equal to 2
Life expectancy greater than or equal to 3 months as determined by treating physician.
Subjects must have adequate organ and marrow at screening as defined below:
peripheral neutrophils >500/µL prior to start of treatment
hemoglobin ≥8 g/dL
Platelets greater than or equal to 50,000 mcL
aspartate aminotransferase (AST)/Alanine aminotransferase (ALT) < 5 × upper limit of normal (ULN
Total bilirubin less than or equal to 1.5 x upper limit of normal (ULN)
Creatinine clearance greater than or equal to 50 mL/min (Cockcroft-Gault)
Exclusion Criteria:
Currently receiving treatment in another investigational device or drug study, or less than 30 days between ending treatment on another investigational device or drug study(ies) and start of IP treatment. Other investigational procedures while participating in this study are excluded.
Known hypersensitivity to immunoglobulins or any other component of the study drug
Subject likely to not be available to complete all protocol required study visits or procedures to the best of the subject and investigator's knowledge
History or evidence of any other clinically significant disorder, condition or disease (with the exception of those outlined above) that, in the opinion of the investigator or Amgen physician, if consulted, would pose a risk to subject safety or interfere with the study evaluation procedures or completion.
Subjects who have had treatments with anti-cancer agents including rituximab or obinutuzumab and/or other monoclonal antibody or radioimmunotherapy within 6 weeks before the starting IP treatment.
Autologous stem cell transplantation within 12 weeks before the starting IP treatment or past history of allogeneic stem cell transplantation.
Subjects who have received anti-CD 19 targeted therapies, chimeric antigen receptor T-cell or other cellular therapies for the treatment of their lymphoma .
Subjects with suspected or known brain metastases should be excluded from this clinical study because of their poor prognosis and because they often develop progressive neurologic dysfunction that would confound the evaluation of neurologic and other adverse events.
Infection with human immunodeficiency virus (HIV) or chronic infection with hepatitis B virus or hepatitis C virus.
History of or current relevant central nervous system pathology such as epilepsy, recurrent seizures, paresis, aphasia, apoplexia, severe brain injuries, cerebellar disease, organic brain syndrome or psychosis.
History of malignancy other than their lymphoma with the exception of:
Malignancy treated with curative intent and with no known active disease present for ≥ 3 years before enrollment and felt to be at low risk for recurrence by the treating physician.
Adequately treated non-melanoma skin cancer or lentigo maligna without evidence of disease.
Adequately treated cervical carcinoma in situ without evidence of disease.
Adequately treated breast ductal carcinoma in situ without evidence of disease
Prostatic intraepithelial neoplasia without evidence of prostate cancer.
Adequately treated urothelial papillary noninvasive carcinoma or carcinoma in situ.
Uncontrolled intercurrent illness including, but not limited to, ongoing or uncontrolled systemic fungal bacteria, viral, or other infection, symptomatic congestive heart failure, unstable angina pectoris, cardiac arrhythmia, or psychiatric illness/social situations that would limit compliance with study requirements.
A female who is pregnant or breastfeeding or planning to become pregnant or breastfeed during treatment and for an additional 48 hours (Period 1) or 96 hours (Period 2), respectively, after the last dose of blinatumomab (Female subjects of childbearing potential should only be included in the study after a confirmed menstrual period and a negative highly sensitive urine or serum pregnancy test).
A female of childbearing potential unwilling to use highly effective method of contraception during treatment and for an additional 48 hours (Period 1) or 96 hours (Period 2), respectively, after the last dose of blinatumomab.
De-identified individual patient data for variables necessary to address the specific research question in an approved data sharing request.
Types
Study Protocol
Statistical Analysis Plan (SAP)
Informed Consent Form (ICF)
Clinical Study Report (CSR)
Time Frame
Data sharing requests relating to this study will be considered beginning 18 months after the study has ended and either 1) the product and indication (or other new use) have been granted marketing authorization in both the US and Europe or 2) clinical development for the product and/or indication discontinues and the data will not be submitted to regulatory authorities. There is no end date for eligibility to submit a data sharing request for this study.
Access Criteria
Qualified researchers may submit a request containing the research objectives, the Amgen product(s) and Amgen study/studies in scope, endpoints/outcomes of interest, statistical analysis plan, data requirements, publication plan, and qualifications of the researcher(s). In general, Amgen does not grant external requests for individual patient data for the purpose of re-evaluating safety and efficacy issues already addressed in the product labelling. Requests are reviewed by a committee of internal advisors, and if not approved, may be further arbitrated by a Data Sharing Independent Review Panel. Upon approval, information necessary to address the research question will be provided under the terms of a data sharing agreement. This may include anonymized individual patient data and/or available supporting documents, containing fragments of analysis code where provided in analysis specifications. Further details are available at the link below.
The participants underwent an initial continuous intravenous (cIV) blinatumomab run-in period (Weeks 1 to 3). The participants received subcutaneous (SC) administration at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, participants received cIV treatment to complete 6 weeks of therapy (Weeks 5 to 6).
Recruitment Details
Of the 39 participants screened, 35 participants were enrolled at 10 centers in the United States, Europe and Australia between 18 September 2017 and 02 September 2021.
Type of Units Analyzed
Not provided
Arm/Group Information
ID
Title
Description
FG000
Blinatumomab Cohort 1
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 112 μq SC administrations every 12 hours (q12h) for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
Periods
Title
Milestones
Reasons Not Completed
Overall Study
Type
Comment
Milestone Data
STARTED
Baseline Characteristics Module
Baseline Analysis Population Description
Outcome Measures Module
Outcome Measures
Adverse Events Module
Frequency Threshold
5
More Info Module
Limitations and Caveats
Not provided
Annotation Section
No data available
No data is available for this block.
Document Section
Large Document Module
Document Has No Statistical Analysis Plan (SAP)
Not provided
Uploaded Document Information
Type
Includes Protocol
Includes SAP
Includes ICF
Document Label
Document Date
Document Uploaded Date
Document File Name
Prot
Yes
No
No
Study Protocol
Feb 25, 2019
Jul 12, 2022
Derived Section
Miscellaneous Info Module
Version Holder
Jul 10, 2026
Removed Countries
Not provided
Submission Tracking
No data available
No data is available for this block.
Condition Browse Module
MeSH Terms
Intervention Browse Module
MeSH Terms
N/A
Intervention Model
Single Group Assignment
Intervention Model Description
Not provided
Primary Purpose
Treatment
Observational Model
Not provided
Time Perspective
Not provided
Masking Info
Masking
None (Open Label)
Masking Description
Not provided
Who Masked
Not provided
Calculated as CL=R0/Css; where R0 is the infusion rate (μg/hr) and Css is the average Css. Both R0 and Css were dose-normalized to 112 μg/day for this calculation.
Once at any timepoint during Day 2 of Weeks 1, 2, 3, 5 and 6
Maximum Observed Concentration (Cmax) of Blinatumomab After SC Administration
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Time at Which Cmax (Tmax) Occurred of Blinatumomab After SC Administration
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Area Under the Concentration-time Curve (AUC) of Blinatumomab After SC Administration for a Dosing Interval t (AUCt)
Estimated using the linear trapezoidal method; where t is a dosing interval. AUC over the dosing interval, t where t is 12 hours for Cohorts 1 and 2, 24 hours for Cohorts 3 and 4, and 48 hours for Cohort 5.
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Minimum Observed Concentration (Cmin) of Blinatumomab After SC Administration
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Apparent Clearance (CL/F) of Blinatumomab After SC Administration
Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Volume of Distribution Based on Terminal Phase (Vz/F) of Blinatumomab After SC Administration
Calculated as Vz/F=CL/F / λz, where λz was the first-order rate constant estimated via linear regression of the terminal log-linear decay phase as determined from the noncompartmental analysis.
Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Terminal Half-life (t1/2,z) of Blinatumomab After SC Administration
Calculated as t1/2,z = ln(2) / λz.
Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Accumulation Ratio of Blinatumomab After SC Administration
Calculated as the ratio of AUCt (last SC dose; Week 4 Day 5) / AUC (first SC dose; Week 4 Day 1).
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Bioavailability (F) of SC Blinatumomab
Calculated as F = (CL * AUCt-ss) / Dose sc.
Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
Maximum Tolerated Dose (MTD) of SC Blinatumomab
The MTD was defined as the highest dose level at which \
Day 1 to Day 7 of Week 4
Number of Participants With Anti-blinatumomab Antibody Formation After SC Administration
Predose at the re-start of cIV infusion (Week 5 Day 1)
Overall Response Rate (ORR) After SC Administration
Percentage of participants achieving ORR (complete response [CR] + partial response [PR]) was determined by best overall response using Cheson criteria:
CR: disappearance of all evidence of disease.
PR: regression of measurable disease and no new sites.
The 95% confidence interval (CI) was calculated using Clopper-Pearson exact CI. Participants were considered as non-responders if there was no response assessment available.
Azienda Socio Sanitaria Territoriale Papa Giovanni XXIII
Bergamo
24127
Italy
Azienda Ospedaliera Universitaria di Bologna Policlinico S Orsola Malpighi
Bologna
40138
Italy
Azienda Socio Sanitaria Territoriale degli Spedali Civili di Brescia
Brescia
25123
Italy
IRCCS Ospedale San Raffaele
Milan
20132
Italy
IRCCS Istituto Clinico Humanitas
Rozzano MI
20089
Italy
Leicester Royal Infirmary
Leicester
LE1 5WW
United Kingdom
FG001
Blinatumomab Cohort 2
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
FG002
Blinatumomab Cohort 3
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 450 μq SC administrations every 24 hours (q24h) for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
FG003
Blinatumomab Cohort 4
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 675 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
FG004
Blinatumomab Cohort 5
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 675 μq SC administrations every 48 hours (q48h) for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
FG0007 subjects
FG0018 subjects
FG0028 subjects
FG0036 subjects
FG0046 subjects
Started Week 4 SC Dosing
FG0006 subjects
FG0017 subjects
FG0027 subjects
FG0036 subjects
FG0045 subjects
Started Week 5-6 cIV Dosing
FG0006 subjects
FG0015 subjects
FG0026 subjects
FG0036 subjects
FG0045 subjects
COMPLETED
Participants who completed investigational product
FG0005 subjects
FG0014 subjects
FG0025 subjects
FG0036 subjects
FG0045 subjects
NOT COMPLETED
FG0002 subjects
FG0014 subjects
FG0023 subjects
FG0030 subjects
FG0041 subjects
Type
Comment
Reasons
Adverse Event
FG0001 subjects
FG0012 subjects
FG0022 subjects
FG0030 subjects
FG0041 subjects
Participant request
FG0000 subjects
FG0012 subjects
FG0020 subjects
FG0030 subjects
FG004
Disease progression
FG0001 subjects
FG0010 subjects
FG0021 subjects
FG0030 subjects
FG004
All enrolled participants.
Type of Units Analyzed
Not provided
Arm/Group Information
ID
Title
Description
BG000
Blinatumomab Cohort 1
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
BG001
Blinatumomab Cohort 2
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
BG002
Blinatumomab Cohort 3
Blinatumomab Cohort 3 The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
BG003
Blinatumomab Cohort 4
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 675 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
BG004
Blinatumomab Cohort 5
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received 675 μq SC administrations q48h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
BG005
Total
Total of all reporting groups
Denominators
Units
Counts
Participants
BG0007
BG0018
BG0028
BG0036
BG0046
BG00535
Baseline Measures
Title
Description
Population Description
Parameter Type
Dispersion Type
Unit of Measure
Calculate Percentage
Denominator Units Selected
Denominators
Classes
Age, Customized
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
18 - 64 years
BG0005
BG0015
BG0023
BG003
Sex: Female, Male
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
Female
BG0003
BG0014
BG002
Ethnicity (NIH/OMB)
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
Hispanic or Latino
BG0001
BG0011
BG002
Race/Ethnicity, Customized
Count of Participants
Participants
Title
Denominators
Categories
American Indian or Alaska Native
Title
Measurements
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
Number of Participants With Dose Limiting-Toxicities (DLTs) After SC Administration
The occurrence of any of the following toxicities during the DLT evaluation period was considered a DLT, if judged by the investigator to be related to the administration of blinatumomab:
Death
Any toxicity, regardless of grade, that lead to a participant's removal from the study by the investigator and/or sponsor
Persistent Common Terminology Criteria for Adverse Events (CTCAE) grade >/= 2 non-hematologic adverse events (AEs) that were deemed intolerable by the participant or the treating physician and that did not respond to appropriate medical management within 5 days and lead to treatment discontinuation
Recurrent grade 2 seizures
All grade 3 and 4 AEs and laboratory abnormalities, which occurred during the SC administration portion of the treatment period with exceptions noted in protocol section 6.2.1.2.3.
DLT analysis set included DLT-evaluable participants who received all (q48h dosing), >/= 4/5 (q24h dosing) or >/= 8/9 (q12h dosing) doses of SC blinatumomab or experienced a DLT during the DLT evaluable period.
Posted
Count of Participants
Participants
Day 1 to Day 7 of Week 4
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG003
Blinatumomab SC Cohort 4
The participants received 675 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG004
Blinatumomab SC Cohort 5
The participants received 675 μq SC administrations q48h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Units
Counts
Participants
OG0006
OG0016
OG0027
OG003
Title
Denominators
Categories
Title
Measurements
OG0000
OG0011
OG0021
OG003
Primary
Number of Participants With DLTs CTCAE Grade ≥ 3 After SC Administration
All toxicities were graded using the CTCAE version 4.0: Grade 1 = mild; Grade 2 = moderate; Grade 3 = severe; Grade 4 = life-threatening; Grade 5 = fatal.
DLT analysis set included DLT-evaluable participants who received all (q48h dosing), >/= 4/5 (q24h dosing) or >/= 8/9 (q12h dosing) doses of SC blinatumomab or experienced a DLT during the DLT evaluable period.
Posted
Count of Participants
Participants
Day 1 to Day 7 of Week 4
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG003
Blinatumomab SC Cohort 4
Primary
Number of Participants With Treatment-emergent Adverse Events (TEAEs) After SC Administration
An AE was defined as any untoward medical occurrence in a clinical study participant. The AE did not necessarily have a causal relationship with study treatment. The definition of AEs included worsening of a pre-existing medical condition.
TEAEs included AEs starting on or after first dose of investigational product and up to the end of study date. All AEs were graded using the CTCAE version 4.0: Grade 1 = mild; Grade 2 = moderate; Grade 3 = severe; Grade 4 = life-threatening; Grade 5 = fatal.
Safety analysis set included participants that were enrolled and received at least 1 dose of blinatumomab.
Posted
Count of Participants
Participants
Day 1 to end of study (approximately 17 weeks)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Secondary
Steady State Serum Concentration (Css) of Blinatumomab After cIV Administration
Summarized as the observed concentrations collected after 5 half-lives after the start of the IV infusion of each dose (i.e., 9, 28 and 112 μg/day).
Pharmacokinetic (PK) analyses set included all participants who received any cIV blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing. Css data during cIV dosing was reported per dose level as pre-specified in statistical analysis plan (SAP) section 10.7.
Posted
Geometric Mean
Geometric Coefficient of Variation
pg/mL
Once at any timepoint during Day 2 of Weeks 1, 2, 3, 5 and 6
ID
Title
Description
OG000
Blinatumomab cIV Before SC Week 1
The participants received 9 μq/day cIV administrations during Week 1.
OG001
Blinatumomab cIV Before SC Week 2
The participants received 28 μq/day cIV administrations during Week 2.
OG002
Blinatumomab cIV Before SC Week 3
The participants received 112 μq/day cIV administrations during Week 3.
Secondary
Systemic Clearance (CL) of Blinatumomab After cIV Administration
Calculated as CL=R0/Css; where R0 is the infusion rate (μg/hr) and Css is the average Css. Both R0 and Css were dose-normalized to 112 μg/day for this calculation.
PK analyses set included all participants who received any cIV blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing. CL data prior to SC dosing was dose-normalized and reported together as pre-specified in SAP section 10.7.
Posted
Geometric Mean
Geometric Coefficient of Variation
L/hr
Once at any timepoint during Day 2 of Weeks 1, 2, 3, 5 and 6
ID
Title
Description
OG000
Blinatumomab cIV Before SC
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day.
OG001
Blinatumomab cIV After SC
After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
Units
Counts
Secondary
Maximum Observed Concentration (Cmax) of Blinatumomab After SC Administration
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing. Descriptive statistics for first SC dose of 675 μg on Week 4 Day 1 were determined using parameter estimates from participants in Cohorts 4 and 5 as pre-specified in SAP section 10.7.
Posted
Geometric Mean
Geometric Coefficient of Variation
pg/mL
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Secondary
Time at Which Cmax (Tmax) Occurred of Blinatumomab After SC Administration
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing. Descriptive statistics for first SC dose of 675 μg on Week 4 Day 1 were determined using parameter estimates from participants in Cohorts 4 and 5 as pre-specified in SAP section 10.7.
Posted
Median
Full Range
hours
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Secondary
Area Under the Concentration-time Curve (AUC) of Blinatumomab After SC Administration for a Dosing Interval t (AUCt)
Estimated using the linear trapezoidal method; where t is a dosing interval. AUC over the dosing interval, t where t is 12 hours for Cohorts 1 and 2, 24 hours for Cohorts 3 and 4, and 48 hours for Cohort 5.
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing. At Week 4 Day 1, AUCt was only reported for SC dosing regimens in Cohorts 1 and 2 as PK sampling was taken only over the 12-hour period following dosing as pre-specified in protocol section 7.1.
Posted
Geometric Mean
Geometric Coefficient of Variation
hr•pg/mL
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Secondary
Minimum Observed Concentration (Cmin) of Blinatumomab After SC Administration
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing. At Week 4 Day 1, Cmin was only reported for SC dosing regimens in Cohorts 1 and 2 as PK sampling was taken only over the 12-hour period following dosing as pre-specified in protocol section 7.1.
Posted
Geometric Mean
Geometric Coefficient of Variation
pg/mL
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Secondary
Apparent Clearance (CL/F) of Blinatumomab After SC Administration
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing.
Posted
Geometric Mean
Geometric Coefficient of Variation
L/hr
Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG003
Secondary
Volume of Distribution Based on Terminal Phase (Vz/F) of Blinatumomab After SC Administration
Calculated as Vz/F=CL/F / λz, where λz was the first-order rate constant estimated via linear regression of the terminal log-linear decay phase as determined from the noncompartmental analysis.
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing.
Posted
Geometric Mean
Geometric Coefficient of Variation
liters
Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Secondary
Terminal Half-life (t1/2,z) of Blinatumomab After SC Administration
Calculated as t1/2,z = ln(2) / λz.
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing.
Posted
Geometric Mean
Geometric Coefficient of Variation
hours
Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG003
Secondary
Accumulation Ratio of Blinatumomab After SC Administration
Calculated as the ratio of AUCt (last SC dose; Week 4 Day 5) / AUC (first SC dose; Week 4 Day 1).
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing.
Posted
Geometric Mean
Geometric Coefficient of Variation
ratio
Week 4 Day 1 (pre-dose and 1, 2, 4, 6, 8 and 12 hours post-dose) and Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Secondary
Bioavailability (F) of SC Blinatumomab
Calculated as F = (CL * AUCt-ss) / Dose sc.
PK analyses set included all participants who received any SC blinatumomab and had at least one PK sample. These participants were evaluated for PK unless significant protocol deviations affected the data analysis or if key dosing, dosing interruption, or sampling information was missing.
Posted
Geometric Mean
Geometric Coefficient of Variation
percent bioavailability
Week 4 Day 5 (pre-dose and 1, 2, 4, 6, 8, 12, 24 and 48 hours post-dose)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG003
Secondary
Maximum Tolerated Dose (MTD) of SC Blinatumomab
The MTD was defined as the highest dose level at which \
DLT analysis set included all DLT-evaluable participants who received all doses (q48h), at least 4/5 doses (q24h) or at least 8/9 doses (q12h) of SC blinatumomab.
Posted
Number
μq
Day 1 to Day 7 of Week 4
ID
Title
Description
OG000
Blinatumomab SC Total
The participants received SC administrations for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Units
Counts
Participants
OG000
Secondary
Number of Participants With Anti-blinatumomab Antibody Formation After SC Administration
Safety analysis set included participants that were enrolled and received at least 1 dose of blinatumomab.
Posted
Count of Participants
Participants
Predose at the re-start of cIV infusion (Week 5 Day 1)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG003
Blinatumomab SC Cohort 4
The participants received 675 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Secondary
Overall Response Rate (ORR) After SC Administration
Percentage of participants achieving ORR (complete response [CR] + partial response [PR]) was determined by best overall response using Cheson criteria:
CR: disappearance of all evidence of disease.
PR: regression of measurable disease and no new sites.
The 95% confidence interval (CI) was calculated using Clopper-Pearson exact CI. Participants were considered as non-responders if there was no response assessment available.
Full analysis set included participants that were enrolled and received at least 1 dose of blinatumomab.
Posted
Number
95% Confidence Interval
percentage of participants
Day 1 to end of study (approximately 17 weeks)
ID
Title
Description
OG000
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG001
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
OG002
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
Time Frame
Day 1 to end of study (approximately 17 weeks)
Description
Safety analysis set included participants that were enrolled and received at least 1 dose of blinatumomab.
All-Cause Mortality Comment
Not provided
Arm/Groups
ID
Title
Description
Deaths (Affected)
Deaths (At Risk)
Serious Events (Affected)
Serious Events (At Risk)
Other Events (Affected)
Other Events (At Risk)
EG000
Blinatumomab cIV Before SC Week 1
The participants received 9 μq/day cIV administrations during Week 1.
1
35
5
35
23
35
EG001
Blinatumomab cIV Before SC Week 2
The participants received 28 μq/day cIV administrations during Week 2.
0
34
5
34
22
34
EG002
Blinatumomab cIV Before SC Week 3
The participants received 112 μq/day cIV administrations during Week 3.
0
33
8
33
23
33
EG003
Blinatumomab SC Cohort 1
The participants received 112 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
0
6
0
6
2
6
EG004
Blinatumomab SC Cohort 2
The participants received 225 μq SC administrations q12h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
0
7
1
7
6
7
EG005
Blinatumomab SC Cohort 3
The participants received 450 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
0
7
1
7
6
7
EG006
Blinatumomab SC Cohort 4
The participants received 675 μq SC administrations q24h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
0
6
0
6
6
6
EG007
Blinatumomab SC Cohort 5
The participants received 675 μq SC administrations q48h for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
0
5
0
5
4
5
EG008
Blinatumomab cIV After SC
After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
1
28
10
28
19
28
EG009
Blinatumomab SC Total
The participants received SC administrations for 5 days at Week 4 followed by a treatment free period of 2 to 3 days.
0
31
2
31
24
31
EG010
Blinatumomab cIV Total
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
2
35
18
35
34
35
EG011
Blinatumomab SC + cIV Total
The participants underwent an initial cIV blinatumomab run-in period (Weeks 1 to 3) in which doses increased each week as follows: Week 1: 9 μq/day; Week 2: 28 μq/day; and Week 3: 112 μq/day. The run-in period was followed by a 12-hour treatment free period. The participants then received SC administrations for 5 days at Week 4 followed by a treatment free period of 2 to 3 days. After the SC administration period, the participants received 112 μq/day cIV blinatumomab during Weeks 5 and 6.
2
35
19
35
35
35
Serious Adverse Events
Term
Organ System
Source Vocabulary
Assessment Type
Notes
Statistical Information
Anaemia
Blood and lymphatic system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG0030 affected6 at risk
EG0040 affected7 at risk
EG0050 affected7 at risk
EG0060 affected6 at risk
EG0070 affected5 at risk
EG0081 affected28 at risk
EG0090 affected31 at risk
EG0101 affected35 at risk
EG0111 affected35 at risk
Febrile neutropenia
Blood and lymphatic system disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Leukopenia
Blood and lymphatic system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Neutropenia
Blood and lymphatic system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Erosive oesophagitis
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Pyrexia
General disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Cytokine release syndrome
Immune system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Dermo-hypodermitis
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Device related sepsis
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Pneumonia
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Sepsis
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Platelet count decreased
Investigations
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Mantle cell lymphoma
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Marginal zone lymphoma refractory
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Aphasia
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Ataxia
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Cognitive disorder
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Coordination abnormal
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Dysarthria
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Hemiparesis
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Motor dysfunction
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Nervous system disorder
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0022 affected33 at risk
EG003
Neurological symptom
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Neurotoxicity
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Seizure
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Confusional state
Psychiatric disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Hallucination
Psychiatric disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Pleural effusion
Respiratory, thoracic and mediastinal disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Hypotension
Vascular disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Other Adverse Events
Term
Organ System
Source Vocabulary
Assessment Type
Notes
Statistical Information
Anaemia
Blood and lymphatic system disorders
MedDRA 24.0
Systematic Assessment
EG0002 affected35 at risk
EG0012 affected34 at risk
EG0021 affected33 at risk
EG0030 affected6 at risk
EG0041 affected7 at risk
EG0051 affected7 at risk
EG0060 affected6 at risk
EG0070 affected5 at risk
EG0083 affected28 at risk
EG0092 affected31 at risk
EG0105 affected35 at risk
EG0116 affected35 at risk
Neutropenia
Blood and lymphatic system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0022 affected33 at risk
EG003
Thrombocytopenia
Blood and lymphatic system disorders
MedDRA 24.0
Systematic Assessment
EG0002 affected35 at risk
EG0011 affected34 at risk
EG0021 affected33 at risk
EG003
Palpitations
Cardiac disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Vertigo
Ear and labyrinth disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Vision blurred
Eye disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Abdominal pain
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0002 affected35 at risk
EG0011 affected34 at risk
EG0021 affected33 at risk
EG003
Abdominal pain upper
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Constipation
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0006 affected35 at risk
EG0013 affected34 at risk
EG0024 affected33 at risk
EG003
Diarrhoea
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0012 affected34 at risk
EG0022 affected33 at risk
EG003
Dyspepsia
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Gastrooesophageal reflux disease
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Nausea
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0013 affected34 at risk
EG0022 affected33 at risk
EG003
Oesophagitis
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Paraesthesia oral
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Vomiting
Gastrointestinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0012 affected34 at risk
EG0020 affected33 at risk
EG003
Administration site erythema
General disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Asthenia
General disorders
MedDRA 24.0
Systematic Assessment
EG0002 affected35 at risk
EG0014 affected34 at risk
EG0022 affected33 at risk
EG003
Fatigue
General disorders
MedDRA 24.0
Systematic Assessment
EG0003 affected35 at risk
EG0012 affected34 at risk
EG0020 affected33 at risk
EG003
Mucosal inflammation
General disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Oedema
General disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Oedema peripheral
General disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Pyrexia
General disorders
MedDRA 24.0
Systematic Assessment
EG0007 affected35 at risk
EG0013 affected34 at risk
EG00211 affected33 at risk
EG003
Cytokine release syndrome
Immune system disorders
MedDRA 24.0
Systematic Assessment
EG0002 affected35 at risk
EG0011 affected34 at risk
EG0021 affected33 at risk
EG003
Cytomegalovirus infection
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Device related infection
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Escherichia infection
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Mucosal infection
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Nasopharyngitis
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Oral herpes
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Respiratory tract infection
Infections and infestations
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Fall
Injury, poisoning and procedural complications
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Infusion related reaction
Injury, poisoning and procedural complications
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0012 affected34 at risk
EG0020 affected33 at risk
EG003
Skin laceration
Injury, poisoning and procedural complications
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Alanine aminotransferase increased
Investigations
MedDRA 24.0
Systematic Assessment
EG0002 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Aspartate aminotransferase increased
Investigations
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Blood alkaline phosphatase increased
Investigations
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0011 affected34 at risk
EG0021 affected33 at risk
EG003
Body temperature increased
Investigations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Platelet count decreased
Investigations
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Weight decreased
Investigations
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Decreased appetite
Metabolism and nutrition disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0021 affected33 at risk
EG003
Folate deficiency
Metabolism and nutrition disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Hyperglycaemia
Metabolism and nutrition disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Hyperkalaemia
Metabolism and nutrition disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Hypocalcaemia
Metabolism and nutrition disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Hypokalaemia
Metabolism and nutrition disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Hyponatraemia
Metabolism and nutrition disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0023 affected33 at risk
EG003
Steroid diabetes
Metabolism and nutrition disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Arthralgia
Musculoskeletal and connective tissue disorders
MedDRA 24.0
Systematic Assessment
EG0002 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Back pain
Musculoskeletal and connective tissue disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0011 affected34 at risk
EG0021 affected33 at risk
EG003
Bone pain
Musculoskeletal and connective tissue disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0012 affected34 at risk
EG0021 affected33 at risk
EG003
Muscle spasms
Musculoskeletal and connective tissue disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Myalgia
Musculoskeletal and connective tissue disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Pain in extremity
Musculoskeletal and connective tissue disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Aphasia
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Cognitive disorder
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Disturbance in attention
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Dizziness
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0012 affected34 at risk
EG0023 affected33 at risk
EG003
Dysarthria
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Dysgraphia
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Encephalopathy
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0021 affected33 at risk
EG003
Headache
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0004 affected35 at risk
EG0013 affected34 at risk
EG0026 affected33 at risk
EG003
Nervous system disorder
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0023 affected33 at risk
EG003
Neurotoxicity
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0003 affected35 at risk
EG0011 affected34 at risk
EG0023 affected33 at risk
EG003
Paraesthesia
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Subdural hygroma
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Tremor
Nervous system disorders
MedDRA 24.0
Systematic Assessment
EG0004 affected35 at risk
EG0011 affected34 at risk
EG0029 affected33 at risk
EG003
Agitation
Psychiatric disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Anxiety
Psychiatric disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Confusional state
Psychiatric disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0022 affected33 at risk
EG003
Insomnia
Psychiatric disorders
MedDRA 24.0
Systematic Assessment
EG0003 affected35 at risk
EG0012 affected34 at risk
EG0020 affected33 at risk
EG003
Irritability
Psychiatric disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Dysphonia
Respiratory, thoracic and mediastinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Dyspnoea
Respiratory, thoracic and mediastinal disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Oropharyngeal pain
Respiratory, thoracic and mediastinal disorders
MedDRA 24.0
Systematic Assessment
EG0001 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Erythema
Skin and subcutaneous tissue disorders
MedDRA 24.0
Systematic Assessment
EG0002 affected35 at risk
EG0011 affected34 at risk
EG0021 affected33 at risk
EG003
Pruritus
Skin and subcutaneous tissue disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Rash
Skin and subcutaneous tissue disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Skin reaction
Skin and subcutaneous tissue disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 at risk
EG003
Astringent therapy
Surgical and medical procedures
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0011 affected34 at risk
EG0020 affected33 at risk
EG003
Hypertension
Vascular disorders
MedDRA 24.0
Systematic Assessment
EG0000 affected35 at risk
EG0010 affected34 at risk
EG0020 affected33 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
The Clinical Trial Agreement generally does not restrict an investigator's discussion of trial results after completion. The Agreement permits Amgen a limited period of time to review material discussing trial results (typically up to 45 days and possible extension). Amgen may remove confidential information, but authors have final control and approval of publication content. For multicenter studies, the investigator agrees not to publish any results before the first multi-center publication.