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dc.contributor.author Cserepes, Mihály
dc.contributor.author Ostoros, Gyula
dc.contributor.author Lohinai, Zoltán
dc.contributor.author Rásó, Erzsébet
dc.contributor.author Barbai, Tamás
dc.contributor.author Tímár, József
dc.contributor.author Rózsás, Anita
dc.contributor.author Moldvay, Judit
dc.contributor.author Kovalszky, Ilona
dc.contributor.author Fábián, Katalin
dc.contributor.author Gyulai, Márton
dc.contributor.author Ghanim, Bahil
dc.contributor.author László, Viktória
dc.contributor.author Thomas, Klikovits
dc.contributor.author Hoda, Mir Alireza
dc.contributor.author Grusch, Michael
dc.contributor.author Berger, Walter
dc.contributor.author Klepetko, Walter
dc.contributor.author Hegedűs, Balázs
dc.contributor.author Döme, Balázs
dc.date.accessioned 2016-08-16T06:55:32Z
dc.date.available 2016-08-16T06:55:32Z
dc.date.issued 2014
dc.identifier 84901787925
dc.identifier.citation pagination=1819-1828; journalVolume=50; journalIssueNumber=10; journalTitle=EUROPEAN JOURNAL OF CANCER;
dc.identifier.uri http://repo.lib.semmelweis.hu//handle/123456789/2950
dc.identifier.uri doi:10.1016/j.ejca.2014.04.001
dc.description.abstract Background: Platinum-based chemotherapy is the most common treatment in advanced-stage lung adenocarcinoma. Because the clinical significance of KRAS mutational status in this setting has not yet been clearly determined, a mutation subtype-specific analysis was performed in the so far largest cohort of Caucasian patients with KRAS mutant advanced-stage lung adenocarcinoma treated with platinum-based chemotherapy. Methods: 505 Caucasian stage III-IV lung adenocarcinoma patients with known amino acid substitution-specific KRAS mutational status and treated with platinum-based chemotherapy were included. The correlations of subtype-specific KRAS mutations with smoking status, progression-free and overall survival (PFS and OS, respectively) and therapeutic response were analysed. Results: Among 338 KRAS wild-type, 147 codon 12 mutant and 20 codon 13 mutant patients, there were no mutation-related significant differences in PFS or OS (P values were 0.534 and 0.917, respectively). Eastern Cooperative Oncology Group (ECOG) status and clinical stage were significant independent prognostic factors. KRAS mutation showed a significant correlation with smoking status (P = 0.018). Importantly, however, G12V KRAS mutant patients were significantly more frequent among never-smokers than all other codon 12 KRAS mutant (G12x) subtypes (P = 0.016). Furthermore, this subgroup tended to have a higher response rate (66% versus 47%; P = 0.077). A modestly longer median PFS was also found in the G12V mutant cohort (233 days; versus 175 days in the G12x group; P = 0.145). Conclusions: While KRAS mutation status per se is neither prognostic nor predictive in stage III-IV lung adenocarcinoma, subtype-specific analysis may indeed identify clinically relevant subgroups of patients that may ultimately influence treatment decisions. © 2014 The Authors.
dc.relation.ispartof urn:issn:0959-8049
dc.title Subtype-specific KRAS mutations in advanced lung adenocarcinoma: A retrospective study of patients treated with platinum-based chemotherapy
dc.type Journal Article
dc.date.updated 2015-12-07T12:43:47Z
dc.language.rfc3066 en
dc.identifier.mtmt 2584900
dc.identifier.wos 000337875800015
dc.identifier.pubmed 24768329
dc.contributor.department SE/AOK/I/I. Sz. Patológiai és Kísérleti Rákkutató Intézet
dc.contributor.department SE/AOK/K/Mellkassebészeti Klinika
dc.contributor.institution Semmelweis Egyetem


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