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Clinical Trial Details — Status: Active, not recruiting

Administrative data

NCT number NCT03215706
Other study ID # CA209-9LA
Secondary ID 2017-001195-35
Status Active, not recruiting
Phase Phase 3
First received
Last updated
Start date August 24, 2017
Est. completion date January 19, 2026

Study information

Verified date January 2024
Source Bristol-Myers Squibb
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study is to determine whether Nivolumab, Ipilimumab combined with chemotherapy is more effective than chemotherapy by itself when treating stage IV NSCLC as the first treatment given for the disease


Recruitment information / eligibility

Status Active, not recruiting
Enrollment 719
Est. completion date January 19, 2026
Est. primary completion date August 16, 2019
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: - Participants with histologically confirmed Stage IV or recurrent NSCLC squamous or non-squamous histology, with no prior systemic anticancer therapy - Eastern Cooperative Oncology Group (ECOG) Performance Status of = 1 - Measurable disease by CT or MRI per response evaluation criteria in solid tumors version 1.1 (RECIST 1.1) criteria - Participants must have PD-L1 IHC testing with results performed by a central laboratory during the screening period Exclusion Criteria: - Participants with known epidermal growth factor receptor (EGFR) mutations which are sensitive to available targeted inhibitor therapy (including, but not limited to, deletions in exon 19 and exon 21 [L858R] substitution mutations) are excluded - Participants with known anaplastic lymphoma kinase (ALK) translocations which are sensitive to available targeted inhibitor therapy are excluded - Participants with untreated CNS metastases are excluded. Participants are eligible if CNS metastases are adequately treated and participants are neurologically returned to baseline (except for residual signs or symptoms related to the CNS treatment) for at least 2 weeks prior to first treatment Other protocol inclusion/exclusion criteria may apply

Study Design


Intervention

Biological:
Ipilimumab
Specified dose on specified day
Nivolumab
Specified dose on specified day
Drug:
Carboplatin
Specified dose on specified day
Paclitaxel
Specified dose on specified day
Pemetrexed
Specified dose on specified day
Cisplatin
Specified dose on specified day

Locations

Country Name City State
Argentina Local Institution - 0014 Ciudad Autónoma de Buenos Aires Buenos Aires
Argentina Local Institution - 0030 Cordoba
Argentina Local Institution - 0028 Rio Cuarto Cordoba
Argentina Local Institution - 0027 Rosario Santa Fe
Argentina Local Institution - 0026 Viedma Rio Negro
Australia Local Institution - 0040 Bedford Park South Australia
Australia Local Institution - 0089 Box Hill Victoria
Australia Local Institution - 0086 Gosford New South Wales
Australia Local Institution - 0036 Heidelberg Victoria
Australia Local Institution - 0078 Murdoch Western Australia
Belgium Local Institution - 0002 Gilly
Belgium Local Institution - 0033 Leuven
Belgium Local Institution - 0001 Roeselare
Brazil Local Institution - 0064 Barretos Sao Paulo
Brazil Local Institution - 0069 Blumenau Santa Catarina
Brazil Local Institution - 0063 Ijui Rio Grande Do Sul
Brazil Local Institution - 0068 Natal RIO Grande DO Norte
Brazil Local Institution - 0067 Porto Alegre Rio Grande Do Sul
Brazil Local Institution - 0066 Rio De Janeiro
Brazil Local Institution - 0065 Sao Jose Do Rio Preto Sao Paulo
Brazil Local Institution - 0070 São Paulo
Canada Local Institution - 0082 Montreal Quebec
Canada Local Institution - 0083 Montreal Quebec
Canada Local Institution - 0090 Montreal Quebec
Canada Local Institution - 0080 Rimouski Quebec
Chile Local Institution - 0059 Santiago Región Metropolitana De Santiago
Chile Local Institution - 0084 Santiago Metropolitana
Chile Local Institution - 0079 Vina Del Mar Valparaiso
China Local Institution - 0113 Beijing
China Local Institution - 0139 Beijing BEI
China Local Institution - 0106 Changchun Jilin
China Local Institution - 0144 Changsha Hunan
China Local Institution - 0146 Haikou Hainan
China Local Institution - 0110 Hangzhou Zhejiang
China Local Institution - 0112 Shanghai
China Local Institution - 0108 Xi'an City Shan3xi
China Local Institution - 0111 Zhejiang Zhejiang
China Local Institution - 0120 Zhengzhou Henan
China Local Institution - 0148 Zhengzhou Henan
France Local Institution - 0010 Bron Rhone Alpes
France Local Institution - 0013 Caen
France Local Institution - 0071 Lille Cedex
France Local Institution - 0009 Lyon Cedex08 Rhône-Alpes
France Local Institution - 0012 Montpellier
France Local Institution - 0035 Nantes
France Local Institution - 0011 Paris Cedex 20
France Local Institution - 0097 Saint-Brieuc
Germany Local Institution - 0073 Berlin
Germany Local Institution - 0016 Gauting
Germany Local Institution - 0072 Grosshansdorf
Germany Local Institution - 0019 Hemer
Germany Local Institution - 0017 Immenhausen
Germany Local Institution - 0074 Magdeburg
Germany Local Institution - 0015 Muenchen
Germany Local Institution - 0018 Yes
Ireland Local Institution - 0021 Dublin
Ireland Local Institution - 0020 Limerick
Italy Ospedale San Luca Lucca
Italy Ospedale San Raffaele Milano
Italy Local Institution - 0043 Napoli
Japan Local Institution - 0131 Akashi-shi Hyogo
Japan Local Institution - 0101 Fukushima-shi Fukushima
Japan Local Institution - 0135 Habikino-shi Osaka
Japan Local Institution - 0119 Himeji-shi Hyogo
Japan Local Institution - 0137 Hiroshima-shi Hiroshima
Japan Local Institution - 0138 Hiroshima-shi Hiroshima
Japan Local Institution - 0115 Kanazawa-shi Ishikawa
Japan Local Institution - 0102 Kitaadachi-gun Saitama
Japan Local Institution - 0104 Kobe-shi Hyogo
Japan Local Institution - 0118 Maebashi-shi Gunma
Japan Local Institution - 0116 Niigata-shi Niigata
Japan Local Institution - 0136 Okayama-shi Okayama
Japan Local Institution - 0103 Osaka-sayama-shi Osaka
Japan Local Institution - 0130 Osaka-shi Osaka
Japan Local Institution - 0128 Ota-shi Gunma
Japan Local Institution - 0127 Sapporo-shi Hokkaido
Japan Local Institution - 0100 Shiwa-gun Iwate
Japan Local Institution - 0132 Ube-shi Yamaguchi
Japan Local Institution - 0114 Yokohama-Shi Kanagawa
Japan Local Institution - 0129 Yokohama-shi Kanagawa
Japan Local Institution - 0134 Yokohama-shi Kanagawa
Mexico Local Institution - 0061 Guadalajara Jalisco
Mexico Local Institution - 0077 La Paz BAJA Californa SUR
Mexico Local Institution - 0075 Veracruz, Veracruz
Poland Local Institution - 0087 Bydgoszcz
Poland Local Institution - 0022 Bytom
Poland Local Institution - 0085 Gdansk
Romania Local Institution - 0034 Bucharest
Romania Local Institution - 0031 Cluj Napoca
Romania Local Institution - 0032 Craiova
Russian Federation Local Institution - 0024 Moscow
Russian Federation Local Institution - 0025 St.petersburg
Spain Local Institution - 0054 A Coruña
Spain Local Institution - 0053 Barcelona
Spain Local Institution - 0052 Madrid
Spain Local Institution - 0055 Malaga
Spain Local Institution - 0056 Valencia
United Kingdom Local Institution - 0050 Guildford
United Kingdom Local Institution - 0049 London
United Kingdom Local Institution - 0048 Tauton
United States Local Institution - 0094 Charleston South Carolina
United States Memorial Health Systems Colorado Springs Colorado
United States Local Institution - 0095 Columbus Ohio
United States Henry Ford Health System Detroit Michigan
United States Baptist MD Anderson Cancer Center Jacksonville Florida
United States Local Institution - 0058 Johnson City New York
United States Local Institution - 0006 Lancaster Pennsylvania
United States Local Institution - 0004 Lexington Kentucky
United States University of Wisconsin Carbone Cancer Center Madison Wisconsin
United States Local Institution - 0029 Marietta Georgia
United States Local Institution - 0098 Mineola New York
United States Local Institution - 0093 Pittsburgh Pennsylvania
United States UPMC Hillman Cancer Center Pittsburgh Pennsylvania
United States Local Institution - 0044 Plainville Connecticut
United States Southwest Regional Cancer Clinic Saint George Utah
United States Local Institution - 0091 Wichita Kansas

Sponsors (1)

Lead Sponsor Collaborator
Bristol-Myers Squibb

Countries where clinical trial is conducted

United States,  Argentina,  Australia,  Belgium,  Brazil,  Canada,  Chile,  China,  France,  Germany,  Ireland,  Italy,  Japan,  Mexico,  Poland,  Romania,  Russian Federation,  Spain,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Overall Survival (OS) OS was defined as the time from randomization to the date of death from any cause. OS was censored on the last date a subject was known to be alive. Survival follow-up was to be conducted every 3 months after participants's off-treatment date. From date of randomization to date of death (assessed up to October 2019, approximately 23 months)
Secondary Progression Free Survival (PFS) by BICR PFS (primary definition) was defined as the time from the randomization date to the date of the first documented tumor progression based on BICR assessment (per RECIST 1.1), or death from any cause, whichever occurred first. Participants who died without a reported prior progression were considered to have progressed on the date of their death. Participants who had not progressed or died were censored on the date of their last evaluable tumor assessment. Participants who did not have any on-study tumor assessments and did not die were censored on the randomization date. Participants who started any palliative local therapy or subsequent anticancer therapy without a prior reported progression were censored at the last evaluable tumor assessment prior to initiation of the palliative local therapy or subsequent anti-cancer therapy, whichever procedure occurred first. From date of randomization until date of documented tumor progression or death due to any cause, whichever occurs first (assessed up to October 2019, approximately 23 months)
Secondary Objective Response Rate (ORR) by BICR ORR was defined as the number of randomized participants with a best overall response (BOR) of confirmed CR or PR based on BICR assessments (using RECIST v1.1 criteria), divided by the number of all randomized participants. BOR was recorded between the date of randomization and the date of objectively documented progression per RECIST 1.1 or the date of initiation of palliative local therapy or the date of initiation of subsequent anti-cancer therapy, whichever occurred first. For participants without documented progression or palliative local therapy or subsequent anti-cancer therapy, all available response designations contributed to the BOR determination. For participants who continued treatment beyond progression, the BOR was determined based on response designations recorded up to the time of the initial RECIST 1.1 defined progression. From date of randomization until date of documented tumor progression or subsequent anti-cancer therapy, whichever occurs first (assessed up to October 2019, approximately 23 months)
Secondary Duration of Response (DoR) DoR was defined as the time between the date of first confirmed documented response (CR or PR) to the date of the first documented BICR-assessed tumor progression (per RECIST 1.1), or death from any cause, whichever occurred first. Participants who started subsequent therapy (including palliative local therapy) without a prior reported progression were censored at the last evaluable tumor assessments prior to initiation of the subsequent anticancer therapy (including palliative local therapy). Participants who died without a reported prior progression were considered to have progressed on the date of their death. For subjects who neither progressed nor died, DoR was censored on the date of their last evaluable tumor assessment. DoR was evaluated for responders (confirmed CR or PR) only. From date of first confirmed response to date of tumor progression (assessed up to October 2019, approximately 23 months)
Secondary Time to Response (TTR) TTR was defined as the time from randomization to the date of the first confirmed documented response (CR or PR), as assessed by the BICR. TTR was evaluated for responders (confirmed CR or PR) only. From date of randomization to date of first confirmed documented response (assessed up to October 2019, approximately 23 months)
Secondary Objective Response Rate (ORR) by BICR by PD-LI Tumor Cell Expression PD-L1 expression was defined as the percent of tumor cells with membrane staining in a minimum of 100 evaluable tumor cells per validated Dako PD-L1 IHC 28-8 pharmDx test. PD-L1 expression was classified as PD-L1 =1% (=1% tumor cells with membrane staining in a minimum of a hundred evaluable tumor cells), PD-L1 < 1% and PD-L1 not quantifiable (without quantifiable PD-L1 expression), PD-L1 expression = 50%, PD-L1 expression 1 to 49% From date of randomization until date of documented tumor progression or subsequent anti-cancer therapy, whichever occurs first (assessed up to October 2019, approximately 23 months)
Secondary PFS by BICR by PD-L1 Tumor Cell Expression PFS (primary definition) was defined as the time from the randomization date to the date of the first documented tumor progression based on BICR assessment (per RECIST 1.1), or death from any cause, whichever occurred first. Participants who died without a reported prior progression were considered to have progressed on the date of their death. Participants who had not progressed or died were censored on the date of their last evaluable tumor assessment. Participants who did not have any on-study tumor assessments and did not die were censored on the randomization date. Participants who started any palliative local therapy or subsequent anticancer therapy without a prior reported progression were censored at the last evaluable tumor assessment prior to initiation of the palliative local therapy or subsequent anti-cancer therapy, whichever procedure occurred first. From date of randomization until date of documented tumor progression or death due to any cause, whichever occurs first (assessed up to October 2019, approximately 23 months)
Secondary OS by PD-L1 Tumor Cell Expression OS was defined as the time from randomization to the date of death from any cause. OS was censored on the last date a subject was known to be alive. Survival follow-up was to be conducted every 3 months after participants's off-treatment date. From date of randomization to date of death (assessed up to October 2019, approximately 23 months)
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