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NCT04810078 Clinical Trial

A Study of Subcutaneous Nivolumab Versus Intravenous Nivolumab in Participants With Previously Treated Clear Cell Renal Cell Carcinoma That is Advanced or Has Spread

Clear Cell Renal Cell Carcinoma Clinical Trial

CheckMate-67T

Official title:
A Phase 3, Open-label, Randomized, Noninferiority Trial of Subcutaneous Formulation of Nivolumab Versus Intravenous Nivolumab in Participants With Advanced or Metastatic Clear Cell Renal Cell Carcinoma Who Have Received Prior Systemic Therapy

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT04810078
Other study ID # CA209-67T
Secondary ID 2020-003655-15U1
Status Recruiting
Phase Phase 3
First received
Last updated
Start date May 24, 2021
Est. completion date January 29, 2026

Study information
Verified date May 2024
Source Bristol-Myers Squibb
Contact BMS Study Connect Contact Center www.BMSStudyConnect.com
Phone 855-907-3286
Email Clinical.Trials@bms.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study is to evaluate the drug levels, efficacy, safety, and tolerability of subcutaneous nivolumab versus intravenous nivolumab in participants with previously treated clear cell renal cell carcinoma that is advanced or has spread. The purpose of this study's substudy is to evaluate drug level biocomparability of subcutaneous nivolumab manufactured using two different manufacturing processes.

Recruitment information / eligibility
Status Recruiting
Enrollment 632
Est. completion date January 29, 2026
Est. primary completion date September 8, 2025
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility For more information regarding Bristol-Myers Squibb Clinical Trial participation, please visit www.BMSStudyConnect.com Inclusion Criteria: - Histological confirmation of renal cell carcinoma (RCC) with a clear cell component, including participants who may also have sarcomatoid features - Advanced RCC (not amenable to curative surgery or radiation therapy) or metastatic RCC (Stage IV) - Measurable disease as defined by Response Evaluation Criteria in Solid Tumor (RECIST) v1.1 criteria within 28 days prior to randomization - Received no more than 2 prior systemic treatment regimens - Intolerance or progression on or after the last treatment regimen received and within 6 months prior to randomization - Karnofsky PS = 70 at screening - Must agree to follow specific methods of contraception, if applicable Exclusion Criteria: - Untreated, symptomatic central nervous system (CNS) metastases - Concurrent malignancy (present during screening) requiring treatment or history of prior malignancy active within 2 years prior to randomization - Active, known, or suspected autoimmune disease - Known human immunodeficiency virus (HIV) positive with an acquired immunodeficiency syndrome (AIDS) defining opportunistic infection within the last year, or a current CD4 count < 350 cells/µL. Participants with HIV are eligible if: 1. They have received established antiretroviral therapy (ART) for at least 4 weeks prior to randomization 2. They continue on ART as clinically indicated while enrolled on study 3. CD4 counts and viral load are monitored per standard of care by a local health care provider 4. Inclusion of participants with HIV should be based on Investigator clinical judgment in consultation with the Medical Monitor NOTE: Testing for HIV must be performed at sites where mandated locally. HIV-positive participants must be excluded where mandated locally - Serious or uncontrolled medical disorders including for example, active severe acute respiratory syndrome coronavirus 2 (SAR-CoV-2) infection within approximately 4 weeks prior to screening. In the case of prior SARS-CoV-2 infection, acute symptoms must have resolved based on investigator clinical judgment and, in consultation with Medical Monitor, there are no sequelae that would place the participant at a higher risk of receiving investigational treatment to be eligible - Prior treatment with an programmed death receptor-1 (anti-PD-1), programmed death ligand-1 (anti-PD-L1), or cytotoxic T-lymphocyte-associated antigen-4 (anti-CTLA-4) antibody, or any other antibody or drug specifically targeting T-cell costimulation or checkpoint pathways - Treatment with any live attenuated vaccine within 30 days of first study treatment Other protocol-defined inclusion/exclusion criteria apply

Study Design

Related Conditions & MeSH terms

Intervention

Biological:
Nivolumab and rHuPH20
Specified dose on specified days
Nivolumab
Specified dose on specified days

Locations
Country Name City State
Argentina Local Institution - 0038 Ciudad Autonoma de BuenosAires Buenos Aires
Argentina Local Institution - 0058 Mar Del Plata Buenos Aires
Argentina Local Institution - 0079 Parana Cordoba
Argentina Local Institution - 0037 Pergamino Buenos Aires
Argentina Cent Priv RMI Rio Cuarto SA II Rio Cuarto Cordoba
Argentina Local Institution - 0056 San Juan
Argentina Local Institution - 0066 Viedma RIO Negro
Brazil Local Institution - 0071 Barretos Sao Paulo
Brazil Local Institution - 0064 Curitiba Parana
Brazil Local Institution - 0011 Ijui RIO Grande DO SUL
Brazil Local Institution - 0107 Ijui Rio Grande Do Sul
Brazil Local Institution - 0039 Porto Alegre RIO Grande DO SUL
Brazil Local Institution - 0090 Rio de Janeiro
Brazil Local Institution - 0070 Sao Jose Do Rio Preto Sao Paulo
Brazil Local Institution - 0081 Sao Paulo
Brazil Local Institution - 0095 Sao Paulo
Brazil Local Institution - 0096 Sao Paulo
Chile Local Institution - 0076 Santiago Metropolitana
Chile Local Institution - 0005 Santiago de Chile Metropolitana
Chile Local Institution - 0104 Santiago de Chile Metropolitana
Chile Local Institution - 0084 Temuco Araucania
Chile Local Institution - 0077 Vina del Mar Valparaiso
Czechia Local Institution - 0063 Brno
Czechia Local Institution - 0036 Hradec Kralove
Czechia Local Institution - 0020 Olomouc
Czechia Local Institution - 0099 Ostrava
Czechia Local Institution - 0010 Prague
Czechia Local Institution - 0106 Praha 8 Liben
Finland Local Institution Jyvaskyla
Finland Local Institution - 0080 Kuopio
Finland Local Institution - 0017 Tampere
Finland Local Institution - 0047 Turku
France Local Institution - 0073 Lyon
France Local Institution Nice cedex 2
France Local Institution - 0051 Suresnes
France Local Institution Toulouse
France Local Institution - 0068 Villejuif
Ireland Local Institution Cork
Ireland Local Institution Dublin
Ireland Local Institution - 0060 Tallaght Dublin
Italy Local Institution - 0033 Cremona
Italy Local Institution - 0008 Firenze
Italy Local Institution - 0027 Meldola
Italy Local Institution - 0018 Milan
Italy Local Institution Milano
Italy Local Institution - 0014 Padova
Italy Local Institution - 0082 Parma
Italy Local Institution - 0092 Pavia
Italy Local Institution Pisa
Italy Local Institution - 0100 Roma
Italy Local Institution - 0091 Rome
Italy Local Institution - 0057 Terni
Mexico Local Institution - 0031 Monterrey Nuevo LEON
Mexico Local Institution - 0103 Monterrey Nuevo LEON
Mexico Local Institution - 0065 Queretaro
Mexico Local Institution - 0085 Queretaro
Mexico Local Institution - 0105 San Luis Potosi
Mexico Local Institution - 0089 Tlalpan Distrito Federal
Mexico Local Institution - 0101 Torreon Coahuila
New Zealand Auckland District Health Board-Auckland City Hospital Auckland
New Zealand Waikato Hospital Hamilton
New Zealand Palmerston North Hospital Palmerston North
Poland Local Institution - 0055 Biala Podlaska
Poland Local Institution - 0062 Bydgoszcz
Poland Local Institution - 0083 Gdansk
Poland Local Institution - 0009 Gliwice
Poland Local Institution - 0021 Krakow
Poland Local Institution - 0098 Krakow
Poland Local Institution - 0001 Poznan
Poland Local Institution - 0023 Warszawa
Portugal Local Institution - 0050 Coimbra
Portugal Local Institution - 0052 Lisboa
Romania Local Institution - 0024 Bucuresti
Romania Local Institution - 0002 Cluj-Napoca
Romania Local Institution - 0040 Cluj-Napoca
Romania Local Institution - 0016 Craiova
Russian Federation SBIH Chelyabinsk Regional Clinical Centre of Oncology and Nuclear Medicine Chelyabinsk
Russian Federation Ivanovo Regional Oncology Dispensary Ivanovo
Russian Federation Hertzen Moscow Oncology Research Center Moscow
Russian Federation Local Institution Moscow
Russian Federation Local Institution Moscow
Russian Federation Local Institution Moscow
Russian Federation Local Institution - 0015 Moscow
Russian Federation Local Institution Nizghiy Novgorod
Russian Federation Budgetary Healthcare Institution of Omsk Region - Clinical Oncological Dispensary Omsk
Russian Federation LLC Eurocityclinic Saint Petersburg
Spain Local Institution - 0048 Barcelona
Spain Local Institution - 0049 Barcelona
Spain Local Institution - 0102 Barcelona
Spain Local Institution - 0067 Madrid
Spain Local Institution - 0072 Madrid
Spain Local Institution - 0074 Madrid
Spain Local Institution - 0075 Madrid
Spain Local Institution - 0032 Sabadell
Spain Local Institution - 0086 Santander
Spain Local Institution - 0059 Sevilla
Turkey Local Institution Adana
Turkey Local Institution - 0026 Ankara
Turkey Local Institution - 0097 Ankara
Turkey Local Institution - 0019 Istanbul
Turkey Local Institution - 0035 Istanbul
Turkey Local Institution Izmir
United States Local Institution - 0025 Buffalo New York
United States Local Institution Chicago Illinois
United States Local Institution - 0088 West Reading Pennsylvania

Sponsors (1)
Lead Sponsor Collaborator
Bristol-Myers Squibb

Countries where clinical trial is conducted

United States,  Argentina,  Brazil,  Chile,  Czechia,  Finland,  France,  Ireland,  Italy,  Mexico,  New Zealand,  Poland,  Portugal,  Romania,  Russian Federation,  Spain,  Turkey, 

Outcome
Type Measure Description Time frame Safety issue
Primary Time-averaged serum concentration over 28 days (Cavgd28) Up to 28 days
Primary Trough serum concentration at steady-state (Cminss) Up to 4 months
Secondary Objective response rate (ORR) by Blinded Independent Central Review (BICR) with a minimum of 6 months follow-up Up to 2 years 6 months
Secondary Trough serum concentration at day 28 (Cmind28) At 28 days
Secondary Maximum serum concentration after the first dose (Cmax1) Up to 7 days
Secondary Peak serum concentration at steady-state (Cmaxss) Up to 4 months
Secondary Steady-state average serum concentration (Cavgss) Up to 4 months
Secondary Trough concentration (Ctrough) At week 17
Secondary Incidence of adverse events (AEs) Up to 2 years 3 months
Secondary Incidence of serious adverse events (SAEs) Up to 2 years 3 months
Secondary Incidence of AEs leading to discontinuation Up to 2 years
Secondary Incidence of deaths Up to 5 years
Secondary Incidence of clinically significant changes in clinical laboratory results: Hematology tests Up to 2 years 3 months
Secondary Incidence of clinically significant changes in clinical laboratory results: Chemistry panel tests Up to 2 years 3 months
Secondary Efficacy parameters: disease control rate (DCR) by BICR with a minimum of 6 months follow-up Up to 2 years 6 months
Secondary Efficacy parameters: DCR by BICR with a minimum of 12 months follow-up Up to 3 years
Secondary Efficacy parameters: DCR by BICR at end of study Up to 5 years
Secondary Efficacy parameters: duration of response (DOR) by BICR with a minimum of 6 months follow-up Up to 2 years 6 months
Secondary Efficacy parameters: DOR by BICR with a minimum of 12 months follow-up Up to 3 years
Secondary Efficacy parameters: DOR by BICR at end of study Up to 5 years
Secondary Efficacy parameters: time to objective response (TTR) by BICR with a minimum of 6 months follow-up Up to 2 years 6 months
Secondary Efficacy parameters: TTR by BICR with a minimum of 12 months follow-up Up to 3 years
Secondary Efficacy parameters: TTR by BICR at end of study Up to 5 years
Secondary Efficacy parameters: progression-free survival (PFS) by BICR with a minimum of 6 months follow-up Up to 2 years 6 months
Secondary Efficacy parameters: PFS by BICR with a minimum of 12 months follow-up Up to 3 years
Secondary Efficacy parameters: PFS by BICR at end of study Up to 5 years
Secondary Efficacy parameters: overall survival (OS) with a minimum of 6 months follow-up Up to 2 years 6 months
Secondary Efficacy parameters: OS with a minimum of 12 months follow-up Up to 3 years
Secondary Efficacy parameters: OS at end of study Up to 5 years
Secondary Efficacy parameters: ORR by BICR with a minimum of 12 months follow-up Up to 3 years
Secondary Efficacy parameters: ORR by BICR at end of study Up to 5 years
Secondary Incidence of anaphylactic, hypersensitivity, and systemic infusion reactions/systemic injection reactions Up to 2 years 3 months
Secondary Incidence of local injection- or infusion-site reactions Up to 2 years 3 months
Secondary Percentage of participants who develop anti-nivolumab antibodies, if applicable Up to 2 years 3 months
Secondary Percentage of participants who develop neutralizing antibodies, if applicable Up to 2 years 3 months
See also
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Terminated NCT01198158 - Everolimus With or Without Bevacizumab in Treating Patients With Advanced Kidney Cancer That Progressed After First-Line Therapy Phase 3
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Recruiting NCT05536141 - A Phase 1 Study of AB521 Monotherapy and Combination Therapies in Renal Cell Carcinoma and Other Solid Tumors Phase 1
Recruiting NCT05119335 - A Study of NKT2152, a HIF2α Inhibitor, in Patients With Advanced Clear Cell Renal Cell Carcinoma Phase 1/Phase 2
Completed NCT01243359 - Sunitinib Malate and Bevacizumab in Treating Patients With Kidney Cancer or Advanced Solid Malignancies Phase 1
Terminated NCT00098618 - Sorafenib and Interferon Alfa in Treating Patients With Locally Advanced or Metastatic Kidney Cancer Phase 2
Recruiting NCT05620134 - Study of JK08 in Patients With Unresectable Locally Advanced or Metastatic Cancer Phase 1/Phase 2
Recruiting NCT06052852 - Study of BDC-3042 as Single Agent and in Combination With Pembrolizumab in Patients With Advanced Malignancies Phase 1/Phase 2
Completed NCT03680521 - Neoadjuvant Sitravatinib in Combination With Nivolumab in Patients With Clear Cell Renal Cell Carcinoma Phase 2
Recruiting NCT06195150 - Overtaking Intra and Inter Tumoral Heterogeneity In Von Hippel-Lindau Related Renal Cancer

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