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Dose-Response Relationships for the Metabolism and Urinary Excretion of Arsenicals in Humans

机译:剂量 - 响应人类代谢与泌尿病的关系

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Two population-based studies of the metabolism and fate of arsenic were performed in individuals who chronically consumed drinking water that contains inorganic arsenic. The first study examined the relationship between the intensity of exposure to inorganic arsenic in drinking water and the urinary excretion of the methylated metabolites, methyl arsenic and dimethyl arsenic. The output of methyl and dimethyl arsenic in urine was found to be relatively constant throughout the day and over a 5-day period. Over a wide range of exposure to inorganic arsenic in drinking water (8-620 μg/l), neither the amount nor percentage of total arsenic in urine that was present as methyl or dimethyl arsenic declined. That is, capacities to methylate inorganic arsenic and to excrete its metabolites in urine were not exceeded over this exposure range. Percentages of the total arsenic in urine that were accounted for by each methylated metabolite varied among individuals. Inter-individual variation could arise from polymorphisms in the enzyme that methylates arsenicals. Further characterization of the enzymology of arsenic methylation in humans will be required to identify sources of interindividual variation. The second study was a pilot study of arsenic and selenium status in chronically exposed individuals. Selenium modifies the distribution, metabolism, retention, and toxicity of inorganic arsenic in many experimental systems; however, few data are available on arsenic and selenium interactions in humans. Although the concentrations of arsenic in blood and urine were correlated, the concentrations of selenium in blood and urine were not. This difference may reflect homeostatic control of selenium metabolism and the absence of such control for arsenic metabolism. When expressed on the basis of body mass, the concentrations of arsenic and selenium in blood, but not in urine, were significantly correlated. Body mass has previously been identified as potential confounder of the analysis of dose-response relationships in individuals chronically exposed to inorganic arsenic.
机译:在长期消耗含有无机砷的饮用水的个体中进行了两种基于砷和砷的命运的基于人群的研究。第一研究检测了饮用水中的无机砷的暴露强度与甲基化代谢物,甲基砷和二甲基砷的尿排泄之间的关系。发现尿液中的甲基和二甲基砷的产出在整天和5天的时间内相对恒定。在饮用水中的无机砷(8-620μg/ L)的各种接触中,尿液中砷的总砷的量也不是甲基或二甲基砷的百分比下降。也就是说,在这种暴露范围内,不超过甲基甲酸甲酯无机砷的能力并排除其尿液中的代谢物。尿液中砷总砷的百分比因各个甲基化代谢物而变化。甲基化砷中的酶中的多态性可能出现各种变异。需要进一步表征人类中砷甲基化酶的酶化,以识别接口变异的来源。第二项研究是在长期暴露的个体中的砷和硒状况的试验研究。硒在许多实验系统中修饰了无机砷的分布,代谢,保留和毒性;然而,很少有数据可以在人类中获得砷和硒互动。虽然血液和尿液中砷的浓度是相关的,但血液和尿液中硒的浓度不存在。这种差异可以反映亚硒酸硒代谢的稳态控制以及砷代谢的缺失。当基于体重表达时,血液中砷和硒的浓度显着相关。之前已被鉴定为潜在的混淆,其分析了长期暴露于无机砷的个体中的剂量 - 反应关系。

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