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Developmentally Restricted Genetic Determinants of Human Arsenic Metabolism: Association between Urinary Methylated Arsenic and CYT19 Polymorphisms in Children

机译:发育受限的人类砷代谢的遗传决定因素:儿童尿甲基化砷与CYT19多态性之间的关联。

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摘要

We report the results of a screen for genetic association with urinary arsenic metabolite levels in three arsenic metabolism candidate genes, PNP, GSTO, and CYT19, in 135 arsenic-exposed subjects from the Yaqui Valley in Sonora, Mexico, who were exposed to drinking water concentrations ranging from 5.5 to 43.3 ppb. We chose 23 polymorphic sites to test in the arsenic-exposed population. Initial phenotypes evaluated included the ratio of urinary inorganic arsenic(III) to inorganic arsenic(V) and the ratio of urinary dimethylarsenic(V) to monomethylarsenic(V) (D:M). In the initial association screening, three polymorphic sites in the CYT19 gene were significantly associated with D:M ratios in the total population. Subsequent analysis of this association revealed that the association signal for the entire population was actually caused by an extremely strong association in only the children (7–11 years of age) between CYT19 genotype and D:M levels. With children removed from the analysis, no significant genetic association was observed in adults (18–79 years). The existence of a strong, developmentally regulated genetic association between CYT19 and arsenic metabolism carries import for both arsenic pharmacogenetics and arsenic toxicology, as well as for public health and governmental regulatory officials.
机译:我们报告了来自墨西哥索诺拉州Yaqui谷的135名暴露于饮用水的砷暴露受试者中三个砷代谢候选基因PNP,GSTO和CYT19与尿砷代谢物水平遗传关联的筛选结果浓度范围从5.5到43.3 ppb。我们选择了23个多态性位点来测试砷暴露人群。评估的初始表型包括尿中无机砷(III)与无机砷(V)的比例以及尿二甲基砷(V)与单甲基砷(V)的比例(D:M)。在最初的关联筛选中,CYT19基因的三个多态性位点与总人群中D:M的比例显着相关。随后对该关联的分析表明,整个人群的关联信号实际上是由仅在CYT19基因型和D:M水平之间的儿童(7-11岁)中的极强关联引起的。从分析中剔除儿童后,成年人(18-79岁)未发现明显的遗传关联。 CYT19与砷代谢之间存在密切的,受发育调节的遗传联系,这对砷的药理遗传学和砷毒理学以及公共卫生和政府监管官员均具有重要意义。

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