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DNA修复基因中的遗传变异可预测肺癌的预后。

Genetic variation in the DNA repair genes is predictive of outcome in lung cancer.

作者信息

Matakidou Athena, el Galta Rachid, Webb Emily L, Rudd Matthew F, Bridle Helen, Eisen Tim, Houlston Richard S

机构信息

Section of Cancer Genetics, Institute of Cancer Research, Sutton, UK.

出版信息

Hum Mol Genet. 2007 Oct 1;16(19):2333-40. doi: 10.1093/hmg/ddm190.

Abstract

To assess whether DNA repair gene variants influence the clinical behaviour of lung cancer we examined the impact of a comprehensive panel of 109 non-synonymous single-nucleotide polymorphisms (nsSNPs) in 50 DNA repair genes on overall survival (OS) in 700 lung cancer patients. Fifteen nsSNPs were associated with OS, significantly greater than that expected (P = 0.04). SNPs associated with prognosis mapped primarily to two repair pathways--nucleotide excision repair (NER): ERCC5 D1104H (P = 0.004); ERCC6 G399D (P = 0.023), ERCC6 Q1413R (P = 0.025), POLE (P = 0.014) and base excision repair: APEX1 D148E (P = 0.028); EXO1 E670G (P = 0.007); POLB P242R (P = 0.018). An increasing number of variant alleles in EXO1 was associated with a poorer prognosis [hazard ratio (HR) = 1.24; P = 0.0009]. A role for variation in NER and BRCA2/FA pathway genes as determinants of OS was provided by an analysis restricted to the 456 patients treated with platinum-based agents. Our data indicate that the pathway-based approach has the potential to generate prognostic markers of clinical outcome.

摘要

为评估DNA修复基因变异是否会影响肺癌的临床行为,我们检测了50个DNA修复基因中的109个非同义单核苷酸多态性(nsSNP)组成的综合面板对700例肺癌患者总生存期(OS)的影响。15个nsSNP与总生存期相关,显著高于预期(P = 0.04)。与预后相关的SNP主要定位于两条修复途径——核苷酸切除修复(NER):ERCC5 D1104H(P = 0.004);ERCC6 G399D(P = 0.023),ERCC6 Q1413R(P = 0.025),POLE(P = 0.014)以及碱基切除修复:APEX1 D148E(P = 0.028);EXO1 E670G(P = 0.007);POLB P242R(P = 0.018)。EXO1中变异等位基因数量的增加与较差的预后相关[风险比(HR)= 1.24;P = 0.0009]。对456例接受铂类药物治疗的患者进行的分析表明,NER和BRCA2/FA途径基因的变异作为总生存期的决定因素发挥了作用。我们的数据表明,基于途径的方法有潜力生成临床结局的预后标志物。

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