Dacarbazine and Ipilimumab vs. Dacarbazine With Placebo in Untreated Unresectable Stage III or IV Melanoma
24 ottobre 2014 aggiornato da: Bristol-Myers Squibb
A Multi-center, Randomized, Double-Blind, Two-Arm, Phase III Study in Patients With Untreated Stage III (Unresectable) or IV Melanoma Receiving Dacarbazine Plus 10 mg/kg Ipilimumab (MDX-010) vs. Dacarbazine With Placebo
The purpose of this clinical research study is to examine the safety and effectiveness (how well the drug works) of two different treatments for patients with melanoma.
One treatment is an investigational compound (a drug that is not currently approved by the United States Food and Drug Administration [FDA]), know as Ipilimumab (also known as MDX-010 or BMS-734016) together with an approved chemotherapy drug called Dacarbazine
Panoramica dello studio
Stato
Completato
Condizioni
Intervento / Trattamento
Descrizione dettagliata
For the extension phase:
Allocation: single arm study; Masking: open label; Intervention Model: Single Group
Tipo di studio
Interventistico
Iscrizione (Effettivo)
681
Fase
- Fase 3
Contatti e Sedi
Questa sezione fornisce i recapiti di coloro che conducono lo studio e informazioni su dove viene condotto lo studio.
Luoghi di studio
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Buenos Aires, Argentina, C1426ANZ
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Buenos Aires, Argentina, C1408INH
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Buenos Aires, Argentina, 1185
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Cordoba, Argentina, X5000AAI
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Santa Fe, Argentina, S3000FFU
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New South Wales
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Coffs Harbour, New South Wales, Australia, 2450
- Local Institution
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Newcastle, New South Wales, Australia, 2300
- Local Institution
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Port Macquarie, New South Wales, Australia, 2444
- Local Institution
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Queensland
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South Brisbane, Queensland, Australia, 4101
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Victoria
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Box Hill, Victoria, Australia, 3128
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Vienna, Austria, 1090
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Brasschaat, Belgio, 2930
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Brussels, Belgio, 1200
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Edegem, Belgio, B-2650
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Gent, Belgio, 9000
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Sao Paulo, Brasile, 01508-010
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Ceara
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Fortaleza, Ceara, Brasile, 60430-230
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Rio Grande Do Sul
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Porto Alegre, Rio Grande Do Sul, Brasile, 90050-170
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Porto Alegre, Rs, Rio Grande Do Sul, Brasile, 90610-000
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Alberta
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Edmonton, Alberta, Canada, T6G 1Z2
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Quebec
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Montreal, Quebec, Canada, H3T 1E2
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Montreal, Quebec, Canada, H1T 2W4
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Saskatchewan
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Saskatoon, Saskatchewan, Canada, S7N 4H4
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Santiago, Chile
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Moscow, Federazione Russa, 115478
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Moscow, Federazione Russa, 105229
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Murmansk, Federazione Russa, 183047
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Ryazan, Federazione Russa, 390011
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Samara, Federazione Russa, 443066
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St Petersburg, Federazione Russa, 198255
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St.-Petersburg, Federazione Russa, 191104
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Stavropol, Federazione Russa, 355047
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Stavropol
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Pyatigorsk, Stavropol, Federazione Russa, 357502
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Bordeaux, Francia, 33075
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Marseille, Francia, 13009
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Paris, Francia, 75010
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Pierre Benite, Francia, 69495
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Villejuif, Francia, 94805
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Cedex
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Brest, Cedex, Francia, 29200
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Cedex 1
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Nantes, Cedex 1, Francia, 44093
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Cedex 2
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Saint Etienne, Cedex 2, Francia, 42055
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Berlin, Germania, 12200
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Heidelberg, Germania, 69120
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Jena, Germania, 07740
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Kiel, Germania, 24105
- Local Institution
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Mannheim, Germania, 68167
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Muenchen, Germania, 81675
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Tubingen, Germania, 72076
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Cork, Irlanda
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Galway, Irlanda
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Dublin 4
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Dublin, Dublin 4, Irlanda
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Jerusalem, Israele, 91120
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Tel Aviv, Israele, 64239
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Genova, Italia, 16128
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Milano, Italia, 20141
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Napoli, Italia, 80131
- Local Institution
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Padova, Italia, 35128
- Local Institution
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Ragusa, Italia, 97100
- Local Institution
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Rome, Italia, 00144
- Local Institution
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Siena, Italia, 53100
- Local Institution
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Oslo
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Montebello, Oslo, Norvegia, 0310
- Local Institution
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Eindhoven, Olanda, 5623 EJ
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Hv Amsterdam, Olanda, 1081
- Local Institution
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Wurzburg, Olanda, 97080
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Gdansk, Polonia, 80-219
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Lodz, Polonia, 93-509
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Lublin, Polonia, 20-090
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Poznan, Polonia, 61-866
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Wroclaw, Polonia, 51-124
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Lisboa, Portogallo, 1099-023
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Avon
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Bristol, Avon, Regno Unito, BS2 8ED
- Local Institution
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Dorset
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Poole, Dorset, Regno Unito, BH15 2JB
- Local Institution
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Essex
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Chelmsford, Essex, Regno Unito, CM1 7ET
- Local Institution
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Greater London
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London, Greater London, Regno Unito, SW3 6JJ
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Merseyside
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Wirral, Merseyside, Regno Unito, CH63 3JY
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Surrey
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Guildford, Surrey, Regno Unito, GU2 7XX
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Olomouc, Repubblica Ceca, 775 20
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Praha, Repubblica Ceca, 128 08
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Barcelona, Spagna, 08036
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Canarias, Spagna, 38320
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Valencia, Spagna, 46014
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Zaragoza, Spagna, 50009
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California
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Anaheim, California, Stati Uniti, 92801
- Pacific Cancer Medical Center
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La Verne, California, Stati Uniti, 91750
- Wilshire Oncology Medical Group Inc
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Los Angeles, California, Stati Uniti, 90025
- The Angeles Clinic and Research Institute
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Palm Springs, California, Stati Uniti, 92262
- Comprehensive Cancer Center
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San Diego, California, Stati Uniti, 92123
- Sharp Clinical Oncology Research
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Connecticut
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Hartford, Connecticut, Stati Uniti, 06105
- Saint Francis Hospital and Medical Center
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Stamford, Connecticut, Stati Uniti, 06902-3628
- Hematology Oncology, P.C.
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Florida
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Jacksonville, Florida, Stati Uniti, 32256
- Cancer Specialists Of North Florida Beaches
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Orlando, Florida, Stati Uniti, 32806
- Orlando Health, Inc. M.D. Anderson Cancer Center Orlando
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Port Saint Lucie, Florida, Stati Uniti, 34952
- Hematology Oncology Associates of the Treasure Coast
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Illinois
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Chicago, Illinois, Stati Uniti, 60637
- University of Chicago
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Normal, Illinois, Stati Uniti, 61761
- Mid-Illinois Hematology/Oncology Associates, Ltd.
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Park Ridge, Illinois, Stati Uniti, 60068
- Oncology Specialists, SC
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Indiana
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Fishers, Indiana, Stati Uniti, 46037
- Central Indiana Cancer Centers
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Indianapolis, Indiana, Stati Uniti, 46202
- Indiana University Cancer Center
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Kansas
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Hutchinson, Kansas, Stati Uniti, 67502
- Hutchinson Clinic, Pa
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Kentucky
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Hazard, Kentucky, Stati Uniti, 41701
- Kentucky Cancer Clinic
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Maryland
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Baltimore, Maryland, Stati Uniti, 21215
- Sinai Hospital of Baltimore
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Baltimore, Maryland, Stati Uniti, 21204
- Greater Baltimore Medical Center
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Massachusetts
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Boston, Massachusetts, Stati Uniti, 02115
- Dana Farber Cancer Institute
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Missouri
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Columbia, Missouri, Stati Uniti, 65203
- Ellis Fischel Cancer Center
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Saint Joseph, Missouri, Stati Uniti, 64507
- St Joseph Oncology Inc
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New Mexico
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Albuquerque, New Mexico, Stati Uniti, 87106
- University of New Mexico Cancer Center
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New York
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New York, New York, Stati Uniti, 10065
- Memorial Sloan Kettering Cancer Center
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North Carolina
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Charlotte, North Carolina, Stati Uniti, 28204
- Blumenthal Cancer Center
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Oregon
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Portland, Oregon, Stati Uniti, 97213
- Providence Portland Medical Center
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Pennsylvania
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Bethlehem, Pennsylvania, Stati Uniti, 18015
- St. Luke's Hospital & Health Network
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South Carolina
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Mount Pleasant, South Carolina, Stati Uniti, 29464
- Lowcountry Hematology & Oncology, Pa
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Tennessee
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Knoxville, Tennessee, Stati Uniti, 37916
- Thompson Cancer Survival Center
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Nashville, Tennessee, Stati Uniti, 37232
- Vanderbilt-Ingram Cancer Ctr
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Texas
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Lubbock, Texas, Stati Uniti, 79410
- Joe Arrington Cancer Research and Treatment Center
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Virginia
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Richmond, Virginia, Stati Uniti, 23226
- Virginia Cancer Institute
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Johannesburg, Sud Africa, 2199
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Eastern Cape
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Port Elizabeth, Eastern Cape, Sud Africa, 6000
- Local Institution
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Gauteng
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Groenkloof, Gauteng, Sud Africa, 0181
- Local Institution
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Pretoria, Gauteng, Sud Africa, 0041
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Saxonworld, Gauteng, Sud Africa, 2196
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Western Cape
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Cape Town, Western Cape, Sud Africa, 7570
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Basel, Svizzera, CH-4031
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Geneva, Svizzera, 1211
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Cherkassy, Ucraina, 18009
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Dnepropetrovsk, Ucraina, 49044
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Lviv, Ucraina, 79031
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Uzhgorod, Ucraina, 88000
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Kaposyar, Ungheria, 7400
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Criteri di partecipazione
I ricercatori cercano persone che corrispondano a una certa descrizione, chiamata criteri di ammissibilità. Alcuni esempi di questi criteri sono le condizioni generali di salute di una persona o trattamenti precedenti.
Criteri di ammissibilità
Età idonea allo studio
18 anni e precedenti (Adulto, Adulto più anziano)
Accetta volontari sani
No
Sessi ammissibili allo studio
Tutto
Descrizione
Inclusion Criteria:
- Informed Consent
- Measurable Disease
- Eastern Cooperative Oncology Group (ECOG) 0 or 1
- Lab / imaging requirements
- Neg for Human Immunodeficiency Virus (HIV), Hepatitis B (HepB), C
- Men and Women > 18 years (16 were allowable)
- Prior therapy restriction (adjuvant only)
Exclusion:
- Pregnant / nursing
- Inadequate contraception
- Brain metastasis
- Primary ocular or mucosal melanoma
Piano di studio
Questa sezione fornisce i dettagli del piano di studio, compreso il modo in cui lo studio è progettato e ciò che lo studio sta misurando.
Come è strutturato lo studio?
Dettagli di progettazione
- Scopo principale: Trattamento
- Assegnazione: Randomizzato
- Modello interventistico: Assegnazione parallela
- Mascheramento: Doppio
Armi e interventi
Gruppo di partecipanti / Arm |
Intervento / Trattamento |
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Sperimentale: Arm A: Ipilimumab and Dacarbazine
In Maintenance phase: Ipilimumab will be continued.
Dacarbazine was given up to Week 22 and is not given in the Maintenance phase
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Intravenous solution; intravenous; 10mg/kg; one dose every 3 weeks for 10 weeks then one dose every 12 weeks starting at Week 24, until disease progression, unacceptable toxicity or withdrawal of consent In Maintenance phase: Only Ipilimumab: 10mg/kg, every 12 weeks will be continued until disease progression
Altri nomi:
Intravenous solution; intravenous; 850 mg/m^2; one dose every 3 weeks for 22 weeks, until disease progression, unacceptable toxicity or withdrawal of consent
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Comparatore attivo: Arm B: Placebo and Dacarbazine
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Intravenous solution; intravenous; 850 mg/m^2; one dose every 3 weeks for 22 weeks, until disease progression, unacceptable toxicity or withdrawal of consent
Intravenous solution; intravenous; 0 mg; one dose every 3 weeks for 10 weeks then one dose every 12 weeks starting at Week 24; until disease progression, unacceptable toxicity or withdrawal of consent
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Cosa sta misurando lo studio?
Misure di risultato primarie
Misura del risultato |
Misura Descrizione |
Lasso di tempo |
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Overall Survival (OS)
Lasso di tempo: Date of randomization to 37 months through 5-year follow-up and up to approximately 76 months
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OS was defined as the time from the date of randomization until the date of death.
Analysis of OS was to be done once 416 deaths had occurred (primary endpoint).
However, analysis occurred at 414 deaths (February 7, 2011), due to operational timing of the study.
Median number of months of OS and associated confidence interval calculated using the method of Brookmeyer and Crowley.
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Date of randomization to 37 months through 5-year follow-up and up to approximately 76 months
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Misure di risultato secondarie
Misura del risultato |
Misura Descrizione |
Lasso di tempo |
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Survival Rate at 1 Year, 18 Months, 2 Years, and 3 Years
Lasso di tempo: Date of randomization to 3 years following randomization
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The survival rate (percentage of participants alive) was defined as the probability that a participant is alive at 1 year (or 18 months, 2 years, or 3 years) following randomization and was estimated via the Kaplan-Meier method.
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Date of randomization to 3 years following randomization
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Disease Control Rate (DCR)
Lasso di tempo: First dose to last tumor assessment prior to subsequent therapy at data cutoff for Primary Endpoint (approximately 5 years)
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DCR=number whose best overall response (BOR) was partial response (PR), complete response (CR) or stable disease (SD), divided by all randomized participants (unevaluable participants included).
Independent review committee assessment.
BOR=date of first dose to last tumor assessment prior to subsequent cancer therapy (including tumor resection, excluding palliative local radiotherapy).
Modified World Health Organization criteria: CR=disappearance of all lesions; no evidence of progressive disease (PD); PR=50% or more decrease in the sum of products of the longest diameter and greatest perpendicular diameter of all index lesions compared with baseline; SD=neither sufficient decrease to qualify for PR nor sufficient increase to qualify for PD; PD=at least 25% increase in sum of products of all index lesions and/or appearance of any new lesions; nonindex lesions: appearance of any new lesions and/or unequivocal progression of nonindex lesions.
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First dose to last tumor assessment prior to subsequent therapy at data cutoff for Primary Endpoint (approximately 5 years)
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Median Number of Months of Progression-free Survival (PFS)
Lasso di tempo: Randomization to date of progression or death to approximately 5 years
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PFS=time between randomization and date of progression or death, whichever occurs first.
Participants who died without reported prior progression were considered to have progressed on date of death.
For those alive and not progressed, PFS was censored on date of last evaluable tumor assessment (TA).
Those who have not died and have no recorded postbaseline TA were censored at randomization.
Those who died without any recorded postbaseline TA were considered to have progressed on date of death.
Evaluation was conducted by both investigator and an independent review committee (IRC), who assessed radiologic imaging studies, photographs of skin lesions, and clinical data.
Progressive disease defined using modified criteria of the World Health Organization: demonstration of at least a 25% increase in the sum of products of all index lesions or the appearance of any new lesions.
For nonindex lesions: appearance of any new lesions or unequivocal progression of nonindex lesions.
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Randomization to date of progression or death to approximately 5 years
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Progression-free Survival (PFS) Rate Truncated at Week 12
Lasso di tempo: Day 78
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PFS rate=probability patient was progression-free at Day 78, calculated as total patients receiving treatment and with an overall response of stable disease (SD), partial response (PR), or complete response (CR) at Week 12, divided by total patients.
For those alive and not progressed at or before Week 12, PFS censored on date of last evaluable tumor assessment (TA) at or before Week 12.
Those with an assessment of PD prior to Week 12 and subsequent assessment of SD, PR, or CR at Week 12 were called progression-free at Week 12.
Those with no recorded postbaseline TA dated on or before Day 109, and who had not died on or before Day 109, were censored at randomization.
PD=at least 25% increase in sum of products of all index lesions or appearance of any new lesions.
Both an investigator and independent review committee (IRC) assessed radiologic imaging studies, photographs of skin lesions, and clinical data.
IRC assessment was considered primary over that of the investigators.
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Day 78
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Best Overall Response Rate (BORR)
Lasso di tempo: First dose to last tumor assessment at data cutoff for primary endpoint (approximately 5 years)
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BORR=number with Best Overall Response (BOR) of complete response (CR) or partial response (PR), divided by total number of randomized patients.
BOR=date of first dose to the last tumor assessment prior to subsequent cancer therapy (including tumor resection surgery but excluding palliative local radiotherapy for bone lesions).
Independent review committee assessment.
Modified criteria of the World Health Organization (mWHO): CR=disappearance of all lesions; no evidence of progressive disease; PR=50% or greater decrease in the sum of products of the longest diameter and greatest perpendicular diameter of all index lesions compared with baseline.
Immune-related (ir) response criteria (irRC) assess tumor response in patients on immunotherapy: irCR=disappearance of all lesions in 2 consecutive observations at least 4 weeks apart; irPR=50% or greater decrease in total measureable tumor burden compared with peak in 2 observations at least 4 weeks apart.
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First dose to last tumor assessment at data cutoff for primary endpoint (approximately 5 years)
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Duration of Response (DOR): Randomized Participants With Response of Complete Response (CR) or Partial Response (PR)
Lasso di tempo: Day of CR or PR to day of PD or death up to data cutoff for primary endpoint (approximately 5 years)
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DOR defined in those with Best Overall Response (BOR)=CR or PR per independent review committee (IRC) as time between date of response of confirmed CR or PR, whichever occurred first, and date of PD or death.
If PR assessed before CR, DOR confirmed at earlier time-point showing PR.
Modified criteria of the World Health Organization (mWHO): CR=disappearance of all lesions;no evidence of PD; PR=50% or greater decrease in the sum of products of longest and greatest perpendicular diameters (SPD) of all index lesions compared with baseline.
PD=an increase of 25% or greater in SPD of index lesions compared with the smallest recorded sum, or appearance of 1 or more new lesions.
Immune-related response criteria (irRC): SD=50% decrease in total measurable tumor burden compared with peak cannot be established nor 25% increase compared with nadir, in absence of unequivocal progression of nonindex lesions.
Unconfirmed immune-related (ir) CR, irPR, or irPD=irSD.
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Day of CR or PR to day of PD or death up to data cutoff for primary endpoint (approximately 5 years)
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Time to Response: All Randomized Participants With Response to Treatment
Lasso di tempo: First dose to date of BOR up to data cutoff for primary endpoint (approximately 5 years)
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Time to response was defined as the time between the first dose of study therapy and the date when measurement criteria were met for Best Overall Response (BOR) of partial response (PR) or complete response (CR), whichever occurred first, per independent review committee.
Note that if an overall response of PR occurred before confirmation of CR, the time to response endpoint was not determined by the time that the BOR of CR was shown but rather by the earlier time point showing PR.
Modified criteria of the World Health Organization: CR=disappearance of all lesions; no evidence of progressive disease (PD); PR=50% or more decrease in the sum of products of the longest and greatest perpendicular diameters (SPD) of all index lesions compared with baseline; PD=an increase of 25% or greater in the SPD of index lesions compared with the smallest recorded sum, or the appearance of 1 or more new lesions.
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First dose to date of BOR up to data cutoff for primary endpoint (approximately 5 years)
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Duration of Stable Disease (SD): Randomized Participants With Stable Disease
Lasso di tempo: Week 12 to date of disease progression or death up to data cutoff for primary endpoint (approximately 5 years)
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Duration of SD was defined in those whose Best Overall Response (BOR) was SD, per independent review committee (IRC) as the time between Week 12 and date of progressive disease (PD) or death , whichever occurs first.
For those who underwent tumor resection following Week 12 but prior to PD, duration of SD was censored on date of last evaluable tumor assessment (TA) prior to resection.
For those with BOR of SD at Week 12, date of PD was used in analysis of duration of SD.
For those with BOR=SD who have not subsequently progressed and who remain alive, duration of SD censored on date of last evaluable TA.
Modified criteria of the World Health Organization (mWHO): SD=insufficient decrease to qualify for partial response or sufficient increase to qualify for PD; PD=an increase of 25% or more in sum of products of longest diameter and greatest perpendicular diameter of index lesions compared with smallest recorded sum, or appearance of 1 or more new lesions.
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Week 12 to date of disease progression or death up to data cutoff for primary endpoint (approximately 5 years)
|
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Percentage of Participants With Brain Metastasis-Free Survival at Time of Data Cutoff
Lasso di tempo: Date of randomization up to data cutoff for primary endpoint (approximately 5 years)
|
Brain metastasis-free survival was defined as the time from randomization to the date of progression with a new lesion located in the brain.
New brain lesions prior to Week 12 constituted a progression event (unlike main progression-free survival analysis).
A participant who dies without documentation of a brain lesion was considered to have progressed with brain metastasis on the date of death.
Participants who are free of brain metastasis were censored on the date of their last tumor assessment.
An independent review committee evaluated images of participants with clinical symptoms to determine the number of those free of brain metastasis.
The brain metastasis-free status was reported as a percent of participants (n/N), where n= participants with metastasis-free brains at data cutoff for the Primary Endpoint and N= randomized participants.
A 2-sided Clopper and Pearson confidence interval was performed.
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Date of randomization up to data cutoff for primary endpoint (approximately 5 years)
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Number of Participants With Adverse Events (AEs), Drug-related AEs, AEs Leading to Discontinuation, Serious Adverse Events (SAEs), Drug-related SAEs, Drug-related Hypersensitivity, Immune-related AEs/SAEs, and Inflammatory AEs/SAEs
Lasso di tempo: Week 1 (First Dose) to 70 days after last dose of study up to data cutoff for primary endpoint (approximately 5 years)
|
AE=any new undesirable symptom, sign, clinically significant laboratory abnormality, or medical condition occurring after starting study treatment, even if the event was not considered to be drug-related.
SAE=a medical event that at any dose results in death, persistent or significant disability/incapacity, or drug dependency/abuse; is life-threatening, an important medical event, or a congenital anomaly/birth defect; or requires or prolongs hospitalization.
Treatment-related=having certain, probable, possible, or missing relationship to study drug.
Grade (Gr) 1=Mild, Gr 2=Moderate, Gr 3=Severe, Gr 4= Potentially Life-threatening or disabling.
Randomization=Day 1; start of treatment (first dose)=Week 1. Summarization time frame is from first dose to 70 days after last dose of study at time of 414 deaths.
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Week 1 (First Dose) to 70 days after last dose of study up to data cutoff for primary endpoint (approximately 5 years)
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Number of Participants With Grade 2-3 and Grade 3-4 Immune-related Adverse Events (irAEs) With Resolution Resolved
Lasso di tempo: Week 1 (first dose) to 70 days after last dose up to data cutoff for primary endpoint (approximately 5 years)
|
irAEs included the categories: gastrointestinal (GI), diarrhea, liver, endocrine, and skin.
Grade 2=moderate adverse events (AEs); minimal, local, or noninvasive intervention indicated.
Grade 3=severe AEs, medically significant but not immediately life-threatening.
Grade 4=life-threatening consequences; urgent intervention indicated.
Resolution is defined as improvement to Grade 1 or less or to the Grade at baseline (prior to treatment).
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Week 1 (first dose) to 70 days after last dose up to data cutoff for primary endpoint (approximately 5 years)
|
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Time to Resolution of Grade 2-3, Grade 3-4 Immune-related Adverse Events (irAEs)
Lasso di tempo: Week 1 (first dose) to 70 days after last dose up to database lock for primary endpoint (approximately 5 years)
|
irAEs included the categories: gastrointestinal (GI), diarrhea, liver, endocrine, and skin.
Grade 2=Moderate adverse events (AEs); minimal, local or noninvasive intervention indicated.
Grade 3=severe AEs, medically significant but not immediately life-threatening.
Grade 4=life-threatening consequences; urgent intervention indicated.
Time to resolution is defined as improvement to Grade 1 or less or to the Grade at baseline (prior to treatment).
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Week 1 (first dose) to 70 days after last dose up to database lock for primary endpoint (approximately 5 years)
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Collaboratori e investigatori
Qui è dove troverai le persone e le organizzazioni coinvolte in questo studio.
Sponsor
Collaboratori
Pubblicazioni e link utili
La persona responsabile dell'inserimento delle informazioni sullo studio fornisce volontariamente queste pubblicazioni. Questi possono riguardare qualsiasi cosa relativa allo studio.
Pubblicazioni generali
- Schadendorf D, Hodi FS, Robert C, Weber JS, Margolin K, Hamid O, Patt D, Chen TT, Berman DM, Wolchok JD. Pooled Analysis of Long-Term Survival Data From Phase II and Phase III Trials of Ipilimumab in Unresectable or Metastatic Melanoma. J Clin Oncol. 2015 Jun 10;33(17):1889-94. doi: 10.1200/JCO.2014.56.2736. Epub 2015 Feb 9.
- Maio M, Grob JJ, Aamdal S, Bondarenko I, Robert C, Thomas L, Garbe C, Chiarion-Sileni V, Testori A, Chen TT, Tschaika M, Wolchok JD. Five-year survival rates for treatment-naive patients with advanced melanoma who received ipilimumab plus dacarbazine in a phase III trial. J Clin Oncol. 2015 Apr 1;33(10):1191-6. doi: 10.1200/JCO.2014.56.6018. Epub 2015 Feb 23.
- Robert C, Thomas L, Bondarenko I, O'Day S, Weber J, Garbe C, Lebbe C, Baurain JF, Testori A, Grob JJ, Davidson N, Richards J, Maio M, Hauschild A, Miller WH Jr, Gascon P, Lotem M, Harmankaya K, Ibrahim R, Francis S, Chen TT, Humphrey R, Hoos A, Wolchok JD. Ipilimumab plus dacarbazine for previously untreated metastatic melanoma. N Engl J Med. 2011 Jun 30;364(26):2517-26. doi: 10.1056/NEJMoa1104621. Epub 2011 Jun 5.
Collegamenti utili
Studiare le date dei record
Queste date tengono traccia dell'avanzamento della registrazione dello studio e dell'invio dei risultati di sintesi a ClinicalTrials.gov. I record degli studi e i risultati riportati vengono esaminati dalla National Library of Medicine (NLM) per assicurarsi che soddisfino specifici standard di controllo della qualità prima di essere pubblicati sul sito Web pubblico.
Studia le date principali
Inizio studio
1 agosto 2006
Completamento primario (Effettivo)
1 gennaio 2011
Completamento dello studio (Effettivo)
1 ottobre 2013
Date di iscrizione allo studio
Primo inviato
8 maggio 2006
Primo inviato che soddisfa i criteri di controllo qualità
9 maggio 2006
Primo Inserito (Stima)
10 maggio 2006
Aggiornamenti dei record di studio
Ultimo aggiornamento pubblicato (Stima)
2 novembre 2014
Ultimo aggiornamento inviato che soddisfa i criteri QC
24 ottobre 2014
Ultimo verificato
1 ottobre 2014
Maggiori informazioni
Termini relativi a questo studio
Parole chiave
Termini MeSH pertinenti aggiuntivi
- Neoplasie per tipo istologico
- Neoplasie
- Tumori neuroectodermici
- Neoplasie, cellule germinali ed embrionali
- Neoplasie, tessuto nervoso
- Tumori neuroendocrini
- Nevi e melanomi
- Melanoma
- Meccanismi molecolari dell'azione farmacologica
- Agenti antineoplastici
- Agenti Antineoplastici, Alchilanti
- Agenti Alchilanti
- Agenti antineoplastici, immunologici
- Inibitori del checkpoint immunitario
- Dacarbazina
- Ipilimumab
Altri numeri di identificazione dello studio
- CA184-024
Queste informazioni sono state recuperate direttamente dal sito web clinicaltrials.gov senza alcuna modifica. In caso di richieste di modifica, rimozione o aggiornamento dei dettagli dello studio, contattare register@clinicaltrials.gov. Non appena verrà implementata una modifica su clinicaltrials.gov, questa verrà aggiornata automaticamente anche sul nostro sito web .
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