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首页> 外文期刊>Molecular Carcinogenesis >Functional genetic variants of XRCC4 XRCC4 and ERCC1 ERCC1 predict survival of gastric cancer patients treated with chemotherapy by regulating the gene expression
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Functional genetic variants of XRCC4 XRCC4 and ERCC1 ERCC1 predict survival of gastric cancer patients treated with chemotherapy by regulating the gene expression

机译:XRCC4 XRCC4和Ercc1 Ercc1的功能遗传变异预测通过调节基因表达治疗化疗治疗的胃癌患者的存活

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摘要

DNA repair protects genomic integrity and may modulate chemotherapy efficacy. Few large‐scale studies have evaluated predictive roles of genetic variants of DNA repair genes in survival of Chinese gastric cancer (GCa) patients treated with chemotherapy. Here, we assessed the roles of 35 single nucleotide polymorphisms (SNPs) in DNA repair genes in survival of 1002 GCa patients, of whom 694 received chemotherapy and 308 did not. Among patients receiving chemotherapy, the ERCC1 rs2298881A allele was associated with a better survival [hazards ratio (HR)?=?0.82, 95% confidence interval (CI)?=?0.69‐0.98; P ?=?0.03], whereas two XRCC4 SNPs were associated with a worse survival (HR?=?1.26, 95% CI?=?1.03‐1.54 for the rs10040363G allele, P ?=?0.02; and HR?=?1.30, 95% CI?=?1.06‐1.59 for the rs2075685T allele, P ?=?0.01). These three SNPs were unique survival predictors for patients treated with chemotherapy ( P? ?0.05 for all) but not for patients without chemotherapy ( P? ?0.05 for all), suggesting that they modulated chemotherapy efficacy. Patients who received chemotherapy and had haplotypes with at least one death‐risk allele in XRCC4 had a poor survival, and the trend for an increase in the number of death‐risk alleles adversely affecting the survival was also observed in an allelic dose‐dependent manner ( P trend ?=?0.001). Further functional analysis revealed that the death‐risk alleles up‐regulated the gene expression, leading to a worse survival as suggested by our meta‐analysis pooling both mRNA microarray data from the GEO database and published data ( ERCC1 : HR?=?1.31 [1.08‐1.58]; P ?=?0.006). These functional genetic variants may independently or jointly affect survival in chemotherapy‐treated GCa patients by modulating the gene expression in the tumors.
机译:DNA修复保护基因组完整性,可调节化疗疗效。很少有大规模研究已经评估了DNA修复基因在化疗治疗治疗的中国胃癌(GCA)患者存活中的DNA修复基因的遗传变异的预测作用。在这里,我们评估了35例单核苷酸多态性(SNP)在1002例GCA患者存活中的DNA修复基因中的作用,其中694名接受化疗和308岁没有。在接受化疗的患者中,ERCC1 RS2298881A等位基因与更好的存活相关[危险比(HR)吗?= 0.82,95%置信区间(CI)?= 0.69-0.98; p?= 0.03],而两种XRCC4 SNP与差的存活率有关(HR?=?1.26,95%CI?=?1.03-1.54为RS10040363G等位基因,P?= 0.02;和HR?=?1.30 ,95%ci?=?1.06-1.59为rs2075685t等位基因,p?= 0.01)。这三种SNP是用化疗治疗的患者的独特存活预测因子(P?β0.05),但不适用于没有化疗的患者(p?&Δ0.05),表明它们调节化疗疗效。接受化疗和XRCC4中至少有一个死亡风险等位基因的患者的存活率差,并且还以等位基因剂量依赖的方式观察到死亡风险等位基因数量增加的趋势(p趋势?= 0.001)。进一步的功能分析表明,死亡风险的成额上调了基因表达,导致我们的META分析汇集来自GEO数据库和公布的数据的MRNA微阵列数据(ERCC1:HR?=?1.31 [ 1.08-1.58]; p?= 0.006)。通过调节肿瘤中的基因表达,这些功能性遗传变体可以独立地或共同影响化疗治疗的GCA患者的存活。

著录项

  • 来源
    《Molecular Carcinogenesis》 |2017年第12期|共12页
  • 作者单位

    Cancer Institute Collaborative Innovation Center for Cancer MedicineFudan University Shanghai;

    Cancer Institute Collaborative Innovation Center for Cancer MedicineFudan University Shanghai;

    Cancer Institute Collaborative Innovation Center for Cancer MedicineFudan University Shanghai;

    Cancer Institute Collaborative Innovation Center for Cancer MedicineFudan University Shanghai;

    Cancer Institute Collaborative Innovation Center for Cancer MedicineFudan University Shanghai;

    Cancer Institute Collaborative Innovation Center for Cancer MedicineFudan University Shanghai;

    Cancer Institute Collaborative Innovation Center for Cancer MedicineFudan University Shanghai;

    Cancer Institute Collaborative Innovation Center for Cancer MedicineFudan University Shanghai;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学;
  • 关键词

    ERCC1; gastric cancer; genetic variants; survival; XRCC4;

    机译:ERCC1;胃癌;遗传变异;存活;XRCC4;

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