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首页> 外文期刊>Journal of the National Cancer Institute >Selenoprotein Gene Variants, Toenail Selenium Levels, and Risk for Advanced Prostate Cancer
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Selenoprotein Gene Variants, Toenail Selenium Levels, and Risk for Advanced Prostate Cancer

机译:硒蛋白基因变异,脚趾甲硒水平和晚期前列腺癌的风险

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摘要

Lower selenium levels have been associated with increased risk of prostate cancer (PCa), and genetic variation in the selenoprotein genes selenoprotein P (SEPP1) and glutathione peroxidase 1 (GPX1) is thought to modify this relationship. We investigated whether the association between toenail selenium levels and advanced PCa risk in the prospective Netherlands Cohort Study is modified by common genetic variation in SEPP1 and GPX1. Toenail clippings were used to determine selenium levels and to isolate DNA for genotyping. This case-cohort study, which included 817 case subjects with advanced PCa and 1048 subcohort members, was analyzed with Cox regression models. All statistical tests were two-sided. Three genetic variants were associated with advanced (stage III/IV or IV) PCa risk: SEPP1 rs7579 (lower risk; P-trend = .01), GPX1 rs17650792 (higher risk; P-trend = .03), and GPX1 rs1800668 (lower risk; P-trend = .005). Toenail selenium levels were inversely associated with advanced PCa risk, independently of common genetic variation in SEPP1 and GPX1.
机译:硒水平降低与前列腺癌(PCa)的风险增加有关,硒蛋白基因硒蛋白P(SEPP1)和谷胱甘肽过氧化物酶1(GPX1)的遗传变异被认为可以改变这种关系。我们调查了前瞻性荷兰队列研究中的趾甲硒水平与晚期PCa风险之间的关联是否被SEPP1和GPX1的常见遗传变异所修饰。脚趾甲修剪用于确定硒水平并分离DNA以进行基因分型。该病例队列研究使用Cox回归模型分析了包括817例晚期PCa和1048个亚队列成员的病例。所有统计检验都是双面的。三种遗传变异与PCa晚期(III / IV或IV期)风险相关:SEPP1 rs7579(较低风险; P-趋势= 0.01),GPX1 rs17650792(较高风险; P-趋势= .03)和GPX1 rs1800668(较低的风险; P趋势= 0.005)。脚趾甲硒水平与晚期PCa风险呈负相关,而与SEPP1和GPX1中常见的遗传变异无关。

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