Return to Clinical Trials Search Results
Randomized, Open-label, Phase 3 Trial of Nivolumab Plus Brentuximab Vedotin Versus Brentuximab Vedotin Alone in Participants With Relapsed Refractory or Ineligible for Autologous Stem Cell Transplant (ASCT) Advanced Stage Classical Hodgkin Lymphoma (CheckMate 812: CHECKpoint Pathway and nivolumab Clinical Trial Evaluation 812)
Primary Objective:
To compare progression free survival of
nivolumab + BV vs BV based on BICR
assessments
Primary Endpoint:
Progression Free Survival (PFS): defined as time from
date of randomization to death, or disease progression.
Secondary Objectives:
To compare the complete response rate of
nivolumab + BV vs BV based on BICR
assessments
To assess objective response rate and duration
of response based on BICR
To assess duration of complete response based
on BICR
To assess overall survival of participants treated
with nivolumab + BV vs BV
To assess PFS based on investigator
assessments
Secondary Endpoints:
Complete Response Rate (CRR): defined as proportion
of participants who have achieved complete response
(Lugano 2014 classification)
Objective Response Rate (ORR): defined as the
proportion of participants who have achieved
complete response or partial response (Lugano 2014
classification)
Duration of response or duration of complete response
(DOR or DOCR): defined as the time from first
response or complete response to the date of initial
objectively documented progression as determined
using the 2014 Lugano classification or death due to
any cause
Overall Survival (OS): defined as the time between the
date of randomization and the date of death.
PFS defined as the above but assessed by investigator.
Tertiary/Exploratory Objectives:
To assess the overall safety and tolerability of
nivolumab in combination with chemotherapy,
as measured by incidence and severity of
adverse events (AEs), serious adverse events
(SAEs), and specific laboratory abnormalities
To assess CRR, BOR, ORR, DOR and DOCR
based on investigator assessments
To investigate the association between
biomarkers in the peripheral blood and tumor
tissue, such as PD-L1 expression, with safety
and efficacy measures
To characterize pharmacokinetics of nivolumab
+ BV and explore exposure-response
relationships
To characterize the immunogenicity of
nivolumab and BV
To evaluate both generic health related quality
of life as assessed by the EQ-5D and cancer
specific quality of life as assessed by the QLQC30,
FACT-Lymphoma and WPAI-GH.
To evaluate the pharmacodynamic activity of
nivolumab + BV combination therapy in the peripheral blood and tumor tissue as measured
by flow cytometry, immunohistochemistry,
soluble factor analysis, and gene expression
(microarray technology, quantitative RT-PCR).
To assess the indeterminate response (IR) as
defined by LYRIC
Tertiary/Exploratory Endpoints:
AEs, study treatment-related AEs, SAEs, and
study treatment-related SAEs will be tabulated
using worst grade per NCI CTCAE v.4.0 criteria
by system organ class and preferred term. Onstudy
lab parameters will be summarized using
worst grade per NCI CTCAE v.4.0 criteria.
CRR, BOR, ORR, DOR and DOCR defined as the
above but assessed by investigator
PD-L1 expression variable of archived tumor
(evaluable, indeterminate, or not evaluable stained
tumor cells) will be assessed in available tumor
specimens obtained at baseline. In addition,
9p24,1 genomic status (polysomy, gain, amplified,
and residual % disomy) may be tested in available
archived tumor samples.
Pharmacokinetic parameters, influence of intrinsic
and extrinsic covariates and potential exposure response
relationship will be characterized using
integrated analyses.
Immunogenicity assessed by ADA positivity
QLQ-C30, FACT-Lymphoma, EuroQol (EQ)-5D-
3L scoring function, and WPAI-GH scoring
algorithm.
Pharmacodynamic activity will be investigated by
ctDNA analysis in the serum and other serum
assessments such as, but not limited to, cytokines,
soluble factors, circulating antibodies, and
proteome analysis. Peripheral blood immune cell
subsets may also be tested.
LYRIC (Lymphoma Response to
Immunomodulatory therapy Criteria) will be used
to assess indeterminate response.
Primary Objective:
To compare progression free survival of
nivolumab + BV vs BV based on BICR
assessments
Primary Endpoint:
Progression Free Survival (PFS): defined as time from
date of randomization to death, or disease progression.
Secondary Objectives:
To compare the complete response rate of
nivolumab + BV vs BV based on BICR
assessments
To assess objective response rate and duration
of response based on BICR
To assess duration of complete response based
on BICR
To assess overall survival of participants treated
with nivolumab + BV vs BV
To assess PFS based on investigator
assessments
Secondary Endpoints:
Complete Response Rate (CRR): defined as proportion
of participants who have achieved complete response
(Lugano 2014 classification)
Objective Response Rate (ORR): defined as the
proportion of participants who have achieved
complete response or partial response (Lugano 2014
classification)
Duration of response or duration of complete response
(DOR or DOCR): defined as the time from first
response or complete response to the date of initial
objectively documented progression as determined
using the 2014 Lugano classification or death due to
any cause
Overall Survival (OS): defined as the time between the
date of randomization and the date of death.
PFS defined as the above but assessed by investigator.
Tertiary/Exploratory Objectives:
To assess the overall safety and tolerability of
nivolumab in combination with chemotherapy,
as measured by incidence and severity of
adverse events (AEs), serious adverse events
(SAEs), and specific laboratory abnormalities
To assess CRR, BOR, ORR, DOR and DOCR
based on investigator assessments
To investigate the association between
biomarkers in the peripheral blood and tumor
tissue, such as PD-L1 expression, with safety
and efficacy measures
To characterize pharmacokinetics of nivolumab
+ BV and explore exposure-response
relationships
To characterize the immunogenicity of
nivolumab and BV
To evaluate both generic health related quality
of life as assessed by the EQ-5D and cancer
specific quality of life as assessed by the QLQC30,
FACT-Lymphoma and WPAI-GH.
To evaluate the pharmacodynamic activity of
nivolumab + BV combination therapy in the peripheral blood and tumor tissue as measured
by flow cytometry, immunohistochemistry,
soluble factor analysis, and gene expression
(microarray technology, quantitative RT-PCR).
To assess the indeterminate response (IR) as
defined by LYRIC
Tertiary/Exploratory Endpoints:
AEs, study treatment-related AEs, SAEs, and
study treatment-related SAEs will be tabulated
using worst grade per NCI CTCAE v.4.0 criteria
by system organ class and preferred term. Onstudy
lab parameters will be summarized using
worst grade per NCI CTCAE v.4.0 criteria.
CRR, BOR, ORR, DOR and DOCR defined as the
above but assessed by investigator
PD-L1 expression variable of archived tumor
(evaluable, indeterminate, or not evaluable stained
tumor cells) will be assessed in available tumor
specimens obtained at baseline. In addition,
9p24,1 genomic status (polysomy, gain, amplified,
and residual % disomy) may be tested in available
archived tumor samples.
Pharmacokinetic parameters, influence of intrinsic
and extrinsic covariates and potential exposure response
relationship will be characterized using
integrated analyses.
Immunogenicity assessed by ADA positivity
QLQ-C30, FACT-Lymphoma, EuroQol (EQ)-5D-
3L scoring function, and WPAI-GH scoring
algorithm.
Pharmacodynamic activity will be investigated by
ctDNA analysis in the serum and other serum
assessments such as, but not limited to, cytokines,
soluble factors, circulating antibodies, and
proteome analysis. Peripheral blood immune cell
subsets may also be tested.
LYRIC (Lymphoma Response to
Immunomodulatory therapy Criteria) will be used
to assess indeterminate response.
Recruitment Status
Past Studies