BRAF codons 594 and 596 mutations identify a new molecular subtype of metastatic colorectal cancer at favorable prognosis

克拉斯医学 V600E型神经母细胞瘤RAS病毒癌基因同源物结直肠癌癌症研究肿瘤科危险系数内科学置信区间突变癌症基因生物遗传学

作者

Chiara Cremolini,Maria Di Bartolomeo,Alessio Amatu,Carlotta Antoniotti,Roberto Moretto,Rosa Berenato,Francesco Perrone,Elena Tamborini,Giuseppe Aprile,Sara Lonardi,Andrea Sartore-Bianchi,Gabriella Fontanini,Massimo Milione,Calogero Lauricella,Salvatore Siena,Alfredo Falcone,Filippo de Braud,Fotios Loupakis,Filippo Pietrantonio

出处

期刊：Annals of Oncology [Elsevier BV]
日期：2015-10-01 卷期号：26 (10): 2092-2097 被引量：135

链接

annalsofoncology.org nih.govdoi.org

标识

DOI：10.1093/annonc/mdv290

摘要

Abstract

Background

While the negative prognostic role of BRAF V600E mutation in metastatic colorectal cancer (mCRC) is well established, the impact of BRAF codons 594 and 596 mutations, occurring in <1% of CRCs, is completely unknown. The present work aims to describe clinical, pathological and molecular features and prognosis of BRAF codons 594 and 596 mutant mCRCs, compared with BRAF V600E mutant and wild-type ones.

Patients and methods

Patients treated for mCRC at three Italian Institutions between October 2006 and October 2014, with available KRAS and NRAS codon 12, 13, 59, 61, 117 and 146 and BRAF codon 594, 596 and 600 mutational status, as detected by means of direct sequencing or matrix assisted laser desorption ionization time-of-flight MassArray, were included.

Results

Ten patients bearing BRAF codons 594 or 596 mutated tumors were identified and compared with 77 and 542 patients bearing BRAF V600E mutated and BRAF wild-type tumors, respectively. While BRAF V600E mutated tumors were more frequently right-sided, mucinous and with peritoneal spread, BRAF 594 or 596 mutated were more frequently rectal, nonmucinous and with no peritoneal spread. All BRAF 594 or 596 mutated tumors were microsatellite stable. Patients with BRAF codons 594 or 596 mutated tumors had markedly longer overall survival (OS) when compared with BRAF V600E mutated [median OS: 62.0 versus 12.6 months; hazard ratio: 0.36 (95% confidence interval 0.20–0.64), P = 0.002], both at univariate and multivariate analyses.

Conclusions

BRAF codon 594 or 596 mutated mCRCs are different from BRAF V600E ones in terms of molecular features, pathological characteristics and clinical outcome. This is consistent with preclinical evidences of a kinase inactivating effect of these mutations. The role of CRAF in transducing the intracellular signal downstream BRAF 594 or 596 mutated proteins opens the way to further preclinical investigation.