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首页> 外文期刊>Cancer epidemiology, biomarkers and prevention: A publication of the American Association for Cancer Research >High-order interactions among genetic variants in DNA base excision repair pathway genes and smoking in bladder cancer susceptibility.
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High-order interactions among genetic variants in DNA base excision repair pathway genes and smoking in bladder cancer susceptibility.

机译:DNA碱基切除修复途径基因的遗传变异与吸烟对膀胱癌易感性之间的高级相互作用。

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摘要

Cancer is a common multifactor human disease resulting from complex interactions between many genetic and environmental factors. In this study, we used a multifaceted analytic approach to explore the relationship between eight single nucleotide polymorphisms in base excision repair (BER) pathway genes, smoking, and bladder cancer susceptibility in a hospital-based case-control study. Overall, we did not find an association between any single BER gene single nucleotide polymorphism and bladder cancer risk. However, in stratified analysis, the OGG1 S326C variant genotypes in ever smokers (odds ratio, 0.74; 95% confidence interval, 0.56-0.99) and ADP-ribosyltransferase (ADPRT) V762A variant genotypes in never smokers (odds ratio, 0.58; 95% confidence interval, 0.37-0.91) conferred a significantly reduced risk. Using logistic regression, we observed that there was a two-way interaction between ADPRT V762A and smoking status. We next used classification and regression tree analysis to explore high-order gene-gene and gene-environment interactions. We found that smoking is the most important influential factor for bladder cancer risk. Consistent with the above findings, we found that the ADPRT V762A was only significantly involved in bladder cancer risk in never smokers and the OGG1 S326C was only significantly involved in ever smokers. We also observed gene-gene interactions among OGG1 S326C, XRCC1 R194W, and MUTYH H335Q in ever smokers. Using multifactor dimensionality reduction approach, the four-factor model, including smoking status, OGG1 S326C (rs1052133), APEX1 D148E (rs3136820), and ADPRT762 (rs1136410), had the best ability to predict bladder cancer risk with the highest cross-validation consistency (100%) and the lowest prediction error (37.02%; P < 0.001). These results support the hypothesis that genetic variants in BER genes contribute to bladder cancer risk through gene-gene and gene-environmental interactions.
机译:癌症是一种常见的多因素人类疾病,是由许多遗传和环境因素之间复杂的相互作用导致的。在这项研究中,我们在医院为基础的病例对照研究中,使用了多方面的分析方法来探索碱基切除修复(BER)通路基因中的八个单核苷酸多态性,吸烟与膀胱癌易感性之间的关系。总体而言,我们未发现任何单个BER基因单核苷酸多态性与膀胱癌风险之间存在关联。然而,在分层分析中,曾经吸烟者的OGG1 S326C变异基因型(几率,0.74; 95%置信区间,0.56-0.99)和从未吸烟者的ADP-核糖基转移酶(ADPRT)V762A变异基因型(几率,0.58; 95%)置信区间0.37-0.91)可以显着降低风险。使用逻辑回归,我们观察到ADPRT V762A与吸烟状况之间存在双向相互作用。接下来,我们使用分类和回归树分析来探索高阶基因-基因和基因-环境的相互作用。我们发现吸烟是膀胱癌风险的最重要影响因素。与上述发现一致,我们发现ADPRT V762A仅在从不吸烟者中显着参与膀胱癌风险,而OGG1 S326C仅从吸烟者中显着参与。我们还观察到了吸烟者中OGG1 S326C,XRCC1 R194W和MUTYH H335Q之间的基因-基因相互作用。使用多因素降维方法,包括吸烟状况,OGG1 S326C(rs1052133),APEX1 D148E(rs3136820)和ADPRT762(rs1136410)的四因素模型具有最佳的预测膀胱癌风险的能力,并且具有最高的交叉验证一致性(100%)和最低的预测误差(37.02%; P <0.001)。这些结果支持这样的假设,即BER基因中的遗传变异通过基因-基因和基因-环境相互作用而导致膀胱癌的风险。

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