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Please use this identifier to cite or link to this item: https://ahro.austin.org.au/austinjspui/handle/1/16115
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dc.contributor.authorLong, Georgina V-
dc.contributor.authorWeber, Jeffrey s-
dc.contributor.authorInfante, Jeffrey R-
dc.contributor.authorKim, Kevin B-
dc.contributor.authorDaud, Adil-
dc.contributor.authorGonzalez, Rene-
dc.contributor.authorSosman, Jeffrey A-
dc.contributor.authorHamid, Omid-
dc.contributor.authorSchuchter, Lynn-
dc.contributor.authorCebon, Jonathan S-
dc.contributor.authorKefford, Richard F-
dc.contributor.authorLawrence, Donald P-
dc.contributor.authorKudchadkar, Ragini-
dc.contributor.authorBurris, Howard A-
dc.contributor.authorFalchook, Gerald S-
dc.contributor.authorAlgazi, Alain-
dc.contributor.authorLewis, Karl-
dc.contributor.authorPuzanov, Igor-
dc.contributor.authorIbrahim, Nageatte-
dc.contributor.authorSun, Peng-
dc.contributor.authorCunningham, Elizabeth-
dc.contributor.authorKline, Amy S-
dc.contributor.authorDel Buono, Heather-
dc.contributor.authorMcDowell, Diane Opatt-
dc.contributor.authorPatel, Kiran-
dc.contributor.authorFlaherty, Keith T-
dc.date2016-01-25-
dc.date.accessioned2016-08-04T07:01:15Z-
dc.date.available2016-08-04T07:01:15Z-
dc.date.issued2016-03-10-
dc.identifier.citationJournal of Clinical Oncology 2016; 34(8): 871-878en_US
dc.identifier.urihttps://ahro.austin.org.au/austinjspui/handle/1/16115-
dc.description.abstractPurpose: To report the overall survival (OS) and clinical characteristics of BRAF inhibitor–naive long-term responders and survivors treated with dabrafenib plus trametinib in a phase I and II study of patients with BRAF V600 mutation–positive metastatic melanoma. Methods: BRAF inhibitor–naive patients treated with dabrafenib 150 mg twice daily plus trametinib 2 mg daily (the 150/2 group) from the non–randomly assigned (part B) and randomly assigned (part C) cohorts of the study were analyzed for progression-free and OS separately. Baseline characteristics and factors on treatment were analyzed for associations with durable responses and OS. Results: For BRAF inhibitor–naive patients in the 150/2 groups (n = 78), the progression-free survival at 1, 2, and 3 years was 44%, 22%, and 18%, respectively, for part B (n = 24) and 41%, 25%, and 21%, respectively, for part C (n = 54). Median OS was 27.4 months in part B and 25 months in part C. OS at 1, 2, and 3 years was 72%, 60%, and 47%, respectively, for part B and 80%, 51%, and 38%, respectively, for part C. Prolonged survival was associated with metastases in fewer than three organ sites and lower baseline lactate dehydrogenase. OS at 3 years was 62% in patients with normal baseline lactate dehydrogenase and 63% in patients with a complete response. Conclusion: Dabrafenib plus trametinib results in a median OS of more than 2 years in BRAF inhibitor–naive patients with BRAF V600 mutation–positive metastatic melanoma, and approximately 20% were progression free at 3 years. Durable responses occurred in patients with good prognostic features at baseline, which may be predictive.en_US
dc.subjectAntineoplastic combined chemotherapy protocolsen_US
dc.subjectMelanomaen_US
dc.subjectProto-oncogene proteins B-rafen_US
dc.titleOverall survival and durable responses in patients with BRAF V600–mutant metastatic melanoma receiving dabrafenib combined with trametiniben_US
dc.typeJournal Articleen_US
dc.identifier.journaltitleJournal of Clinical Oncologyen_US
dc.identifier.affiliationAustin Health, Heidelberg, Victoria, Australiaen_US
dc.identifier.affiliationMelanoma Institute Australia, North Sydney, NSW, Australiaen_US
dc.identifier.affiliationThe University of Sydney, Sydney, NSW, Australiaen_US
dc.identifier.affiliationMacquarie University, Sydney, NSW, Australiaen_US
dc.identifier.affiliationWestmead Hospital, Westmead, NSW, Australiaen_US
dc.identifier.affiliationMoffitt Cancer Center, Tampa, FL, USAen_US
dc.identifier.affiliationSarah Cannon Research Institute, Nashville, TN, USAen_US
dc.identifier.affiliationCalifornia Pacific Medical Center, San Francisco, CA, USAen_US
dc.identifier.affiliationTennessee Oncology, Nashville, TN, USAen_US
dc.identifier.affiliationUniversity of California, San Francisco, CA, USAen_US
dc.identifier.affiliationThe Angeles Clinic and Research Institute, Los Angeles, CA, USen_US
dc.identifier.affiliationUniversity of Colorado, Boulder, CO, USAen_US
dc.identifier.affiliationSarah Cannon Research Institute at HealthONE, Denver, CO, USAen_US
dc.identifier.affiliationVanderbilt University Medical Center, Nashville, TN, USAen_US
dc.identifier.affiliationUniversity of Pennsylvania Abramson Cancer Center, Phildelphia, PA, USAen_US
dc.identifier.affiliationMerck, USAen_US
dc.identifier.affiliationGlaxoSmithKline, Philadelphia, PA, USAen_US
dc.identifier.affiliationIncyte Corporation, Wilmington, DE, USAen_US
dc.identifier.affiliationMassachusetts General Hospital Cancer Center, Boston, MA, USAen_US
dc.identifier.pubmedurihttps://pubmed.ncbi.nlm.nih.gov/26811525en_US
dc.identifier.doi10.1200/JCO.2015.62.9345en_US
dc.type.contentTexten_US
dc.type.austinJournal Articleen_US
local.name.researcherCebon, Jonathan S
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
item.grantfulltextnone-
item.cerifentitytypePublications-
item.openairetypeJournal Article-
item.fulltextNo Fulltext-
crisitem.author.deptOlivia Newton-John Cancer Research Institute-
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