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饮酒、乙醇脱氢酶基因变异与肾细胞癌风险。

Alcohol consumption, variability in alcohol dehydrogenase genes and risk of renal cell carcinoma.

机构信息

Department of Health Sciences Research, 4500 San Pablo Road, Jacksonville, FL.

Department of Health Sciences Research, 200 1st St. SW, Rochester, MN.

出版信息

Int J Cancer. 2018 Feb 15;142(4):747-756. doi: 10.1002/ijc.31103. Epub 2017 Oct 28.

DOI:10.1002/ijc.31103
PMID:29023769
Abstract

Alcohol consumption has been associated inversely with renal cell carcinoma (RCC) risk; however, no study has examined effect modification by germline variation in alcohol-metabolizing genes. We investigated whether the association between alcohol intake and RCC risk is modulated by germline variants in alcohol dehydrogenase genes in a large case-control study. Data from 652 RCC cases and 1,366 non-cancer controls were analyzed. Alcohol intake was assessed using a standardized risk factor questionnaire. Three previously genotyped polymorphisms in ADH6 and ADH7 with the TaqMan assay were examined. Odds ratios (ORs) and 95% confidence interval (CI) were calculated using logistic regression, adjusting for covariates. Compared to non-drinkers, ever consumption of alcohol was associated with lower RCC risk (OR = 0.52, 95% CI = 0.42-0.65). Analysis with cubic spline regression curve showed a "J-shaped" relationship between alcohol drinks/day and RCC risk, such that there was no added benefit against RCC for consumption of more than two drinks/day. We observed effect modification by variation in rs1154454 (ADH7) (p  = 0.007); a per unit increase in alcohol drink/day was associated with 35% lower RCC risk among non-minor allele carriers, a 27% lower risk among those who carry one copy of the minor allele, but no association was observed among those with two copies of the minor allele. These findings indicate that alcohol consumption is associated with lower RCC risk. Consuming more than two drinks a day does not confer additional protection against RCC. The association between alcohol intake and RCC risk appears to be modulated by inter-individual germline variation in alcohol-metabolizing genes.

摘要

饮酒与肾细胞癌(RCC)风险呈负相关;然而,尚无研究探讨酒精代谢基因种系变异对其的影响修饰作用。我们在一项大型病例对照研究中,调查了酒精摄入与 RCC 风险之间的关联是否受酒精脱氢酶基因种系变异的调节。对 652 例 RCC 病例和 1366 例非癌症对照的数据进行了分析。采用标准化危险因素问卷评估饮酒量。使用 TaqMan 检测法检测 ADH6 和 ADH7 中三个先前遗传的多态性。使用逻辑回归,调整协变量后,计算比值比(OR)和 95%置信区间(CI)。与非饮酒者相比,曾饮酒者患 RCC 的风险较低(OR=0.52,95%CI=0.42-0.65)。使用三次样条回归曲线分析表明,酒精摄入量与 RCC 风险之间存在“J 形”关系,即每天饮酒超过两杯并不会增加对 RCC 的预防效果。我们观察到 rs1154454(ADH7)的变异存在效应修饰(p=0.007);每天每增加一杯酒精饮料,非次要等位基因携带者患 RCC 的风险降低 35%,携带一个次要等位基因的风险降低 27%,但未观察到携带两个次要等位基因的患者存在相关性。这些发现表明,饮酒与较低的 RCC 风险相关。每天饮用超过两杯酒并不能额外预防 RCC。饮酒与 RCC 风险之间的关联似乎受个体间酒精代谢基因种系变异的调节。

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