The Impact of <i>EGFR</i> T790M Mutations and <i>BIM</i> mRNA Expression on Outcome in Patients with <i>EGFR</i> -Mutant NSCLC Treated with Erlotinib or Chemotherapy in the Randomized Phase III EURTAC Trial

Carlota Costa(Molecular Oncology (United States)), Miguel Angel Molina(Molecular Oncology (United States)), Ana Drozdowskyj(Molecular Oncology (United States)), Ana Giménez‐Capitán(Molecular Oncology (United States)), Jordi Bertrán-Alamillo(Molecular Oncology (United States)), Niki Karachaliou(Molecular Oncology (United States)), Radj Gervais(Molecular Oncology (United States)), Bartomeu Massutí(Molecular Oncology (United States)), Jia Wei(Molecular Oncology (United States)), Teresa Morán(Molecular Oncology (United States)), Margarita Majem(Molecular Oncology (United States)), Enriqueta Felip(Molecular Oncology (United States)), Enric Carcereny(Molecular Oncology (United States)), Rosario García‐Campelo(Molecular Oncology (United States)), Santiago Viteri(Molecular Oncology (United States)), Miquel Tarón(Molecular Oncology (United States)), Mayumi Ono(Molecular Oncology (United States)), Petros Giannikopoulos(Molecular Oncology (United States)), Trever G. Bivona(Molecular Oncology (United States)), Rafael Rosell(Molecular Oncology (United States))
Clinical Cancer Research
February 3, 2014
10.1158/1078-0432.ccr-13-2233
Cited by 226Open Access
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Abstract

PURPOSE: Concomitant genetic alterations could account for transient clinical responses to tyrosine kinase inhibitors of the EGF receptor (EGFR) in patients harboring activating EGFR mutations. EXPERIMENTAL DESIGN: We have evaluated the impact of pretreatment somatic EGFR T790M mutations, TP53 mutations, and Bcl-2 interacting mediator of cell death (BCL2L11, also known as BIM) mRNA expression in 95 patients with EGFR-mutant non-small-cell lung cancer (NSCLC) included in the EURTAC trial (trial registration: NCT00446225). RESULTS: T790M mutations were detected in 65.26% of patients using our highly sensitive method based on laser microdissection and peptide-nucleic acid-clamping PCR, which can detect the mutation at an allelic dilution of 1 in 5,000. Progression-free survival (PFS) to erlotinib was 9.7 months for those with T790M mutations and 15.8 months for those without, whereas among patients receiving chemotherapy, it was 6 and 5.1 months, respectively (P < 0.0001). PFS to erlotinib was 12.9 months for those with high and 7.2 months for those with low/intermediate BCL2L11 expression levels, whereas among chemotherapy-treated patients, it was 5.8 and 5.5 months, respectively (P = 0.0003). Overall survival was 28.6 months for patients with high BCL2L11 expression and 22.1 months for those with low/intermediate BCL2L11 expression (P = 0.0364). Multivariate analyses showed that erlotinib was a marker of longer PFS (HR = 0.35; P = 0.0003), whereas high BCL2L11 expression was a marker of longer PFS (HR = 0.49; P = 0.0122) and overall survival (HR = 0.53; P = 0.0323). CONCLUSIONS: Low-level pretreatment T790M mutations can frequently be detected and can be used for customizing treatment with T790M-specific inhibitors. BCL2L11 mRNA expression is a biomarker of survival in EGFR-mutant NSCLC and can potentially be used for synthetic lethality therapies.

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