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Toxicogenetic profile and cancer risk in Lebanese

机译:黎巴嫩人的毒物学概况和癌症风险

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摘要

An increasing number of genetic polymorphisms in drug-metabolizing enzymes (DME) were identified among different ethnic groups. Some of these polymorphisms are associated with an increased cancer risk, while others remain equivocal. However, there is sufficient evidence that these associations become significant in populations overexposed to environmental carcinogens. Hence, genetic differences in expression activity of both Phase I and Phase II enzymes may affect cancer risk in exposed populations. In Lebanon, there has been a marked rise in reported cancer incidence since the 1990s. There are also indicators of exposure to unusually high levels of environmental pollutants and carcinogens in the country. This review considers this high cancer incidence by exploring a potential gene-environment model based on available DME polymorphism prevalence, and their impact on bladder, colorectal, prostate, breast, and lung cancer in the Lebanese population. The examined DME include glutathione S-transferases (GST), N-acetyltransferases (NAT), and cytochromes P-450 (CYP). Data suggest that these DME influence bladder cancer risk in the Lebanese population. Evidence indicates that identification of a gene-environment interaction model may help in defining future research priorities and preventive cancer control strategies in this country, particularly for breast and lung cancer.
机译:在不同种族之间发现了越来越多的药物代谢酶(DME)基因多态性。这些多态性中的一些与增加的癌症风险有关,而另一些仍然模棱两可。但是,有足够的证据表明这些关联在过度暴露于环境致癌物的人群中变得很重要。因此,I期和II期酶表达活性的遗传差异可能会影响暴露人群的癌症风险。自1990年代以来,在黎巴嫩,报告的癌症发病率显着上升。该国也有暴露于异常高水平的环境污染物和致癌物的指标。这篇综述通过探讨基于可用DME多态性患病率的潜在基因环境模型及其对黎巴嫩人群膀胱癌,结肠直肠癌,前列腺癌,乳腺癌和肺癌的影响,来考虑这种高癌症发生率。检查的DME包括谷胱甘肽S-转移酶(GST),N-乙酰基转移酶(NAT)和细胞色素P-450(CYP)。数据表明,这些DME影响黎巴嫩人群的膀胱癌风险。有证据表明,确定基因与环境的相互作用模型可能有助于确定该国未来的研究重点和预防性癌症控制策略,尤其是对于乳腺癌和肺癌。

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