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Alcohol and genetic polymorphisms: effect on risk of alcohol-related cancer.

机译:酒精和遗传多态性:对酒精相关癌症风险的影响。

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Public health guidelines aim to limit the consumption of alcoholic beverages worldwide and the subsequent health burden. In particular, alcohol consumption is an avoidable risk factor for cancer. In human beings, ethanol in alcoholic drinks is mainly oxidised in the liver by alcohol dehydrogenases to acetaldehyde, and is further detoxified to acetate by aldehyde dehydrogenases. Functional variants in genes involved in alcohol metabolism result in differences between individuals in exposure to carcinogenic acetaldehyde, suggesting a possible interaction of genetic susceptibility and alcohol exposure in cancer. We reviewed available studies of the combined effects of alcohol drinking and genetic polymorphisms on alcohol-related cancer risk. Most available data were for polymorphisms in alcohol and folate metabolism. We give an overview of published studies on the combined effects of alcohol drinking and polymorphisms in genes for alcohol dehydrogenase (ADH), aldehyde dehydrogenase (ALDH), cytochrome P4502E1, and methylene-tetrahydrofolate reductase on the risk of alcohol-related cancer. Current data lend support to a role of polymorphisms ADH1B and ALDH2 combined with alcohol consumption in cancer. Other available data are insufficient or inconclusive, highlighting the need for additional studies.
机译:公共卫生指南旨在限制全球范围内酒精饮料的消费以及随之而来的健康负担。特别是,饮酒是可避免的癌症危险因素。在人类中,酒精饮料中的乙醇主要在肝脏中被乙醇脱氢酶氧化成乙醛,并进一步被醛脱氢酶解毒成乙酸盐。参与酒精代谢的基因的功能变异会导致致癌乙醛暴露个体之间的差异,这表明癌症中遗传易感性和酒精暴露之间可能存在相互作用。我们回顾了有关饮酒和遗传多态性对酒精相关癌症风险的综合影响的现有研究。大多数可用数据涉及酒精和叶酸代谢的多态性。我们概述了有关饮酒和酒精脱氢酶(ADH),醛脱氢酶(ALDH),细胞色素P4502E1和亚甲基四氢叶酸还原酶基因中多态性对酒精相关癌症风险的已发表研究的概述。当前数据支持多态性ADH1B和ALDH2与饮酒相结合在癌症中的作用。其他可用数据不足或尚无定论,这突出表明需要进行更多研究。

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