首页> 外文期刊>Chemical research in toxicology >Selenium compounds modulate the activity of recombinant rat AsIII-methyltransferase and the methylation of arsenite by rat and human hepatocytes.
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Selenium compounds modulate the activity of recombinant rat AsIII-methyltransferase and the methylation of arsenite by rat and human hepatocytes.

机译:硒化合物调节大鼠和人类肝细胞重组大鼠AsIII-甲基转移酶的活性以及亚砷酸的甲基化。

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摘要

Formation of methylated metabolites is a critical step in the metabolism of inorganic arsenic or selenium. We have previously shown that under conditions of a concurrent exposure sodium selenite inhibits methylation of arsenite by cultured rat hepatocytes. Here, we compare the effects of sodium selenite and mono-, di-, and trimethylated selenium compounds on the methylation of arsenite by purified recombinant rat As(III)-methyltransferase (Cyt19) and by primary rat and human hepatocytes. Among these compounds, sodium selenite was the most potent inhibitor of the methylation of arsenite by the recombinant enzyme (K(i) = 1.4 microM) and by cultured cells. In both systems, methylseleninic acid was an order of magnitude less potent an inhibitor (K(i) = 19.4 microM) than was sodium selenite. Dimethylselenoxide and trimethylselenonium iodide were weak activators of recombinant As(III)-methyltransferase activity but were weak inhibitors of arsenite methylation in hepatocytes. These data suggest that selenite,rather than its methylated metabolites, is responsible for inhibition of arsenite methylation in cultured hepatocytes and that inhibition may involve direct interactions between selenite and As(III)-methyltransferase.
机译:甲基化代谢物的形成是无机砷或硒代谢的关键步骤。先前我们已经表明,在同时暴露的条件下,亚硒酸钠会抑制培养的大鼠肝细胞对亚砷酸的甲基化。在这里,我们比较了亚硒酸钠和单,二和三甲基化硒化合物对纯化的重组大鼠As(III)-甲基转移酶(Cyt19)以及原代大鼠和人类肝细胞对亚砷酸甲基化的影响。在这些化合物中,亚硒酸钠是重组酶(K(i)= 1.4 microM)和培养细胞对亚砷酸甲基化最有效的抑制剂。在这两个系统中,甲基硒酸的抑制剂效能(K(i)= 19.4 microM)都比亚硒酸钠低一个数量级。二甲基硒氧化物和三甲基碘化碘是重组As(III)-甲基转移酶活性的弱激活剂,但是肝细胞中亚砷酸甲基化的弱抑制剂。这些数据表明,亚硒酸盐而不是其甲基化的代谢产物是抑制培养的肝细胞中亚砷酸盐甲基化的原因,并且该抑制作用可能涉及亚硒酸盐与As(III)-甲基转移酶之间的直接相互作用。

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