首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Chromium is the proximate clastogenic species for lead chromate-induced clastogenicity in human bronchial cells.
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Chromium is the proximate clastogenic species for lead chromate-induced clastogenicity in human bronchial cells.

机译:铬是人支气管细胞中铬酸铅诱导的致灭性作用的最接近致裂物。

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Hexavalent chromium (Cr(VI)) is a well-established human lung carcinogen with potentially widespread exposure. Solubility is a key factor in the carcinogenicity of Cr(VI), with the water-insoluble or 'particulate' compounds being the more potent carcinogens. Studies have indicated that the component ions are responsible for their clastogenicity, but it is uncertain whether chromium (Cr), lead (Pb) or some combination of the two is responsible for the clastogenic effects. Accordingly, we compared the clastogenicity of lead chromate (LC) with soluble sodium chromate (SC) and lead glutamate (LG) in WTHBF-6 human lung cells. We found that 1436microM was the maximal intracellular level of Pb after exposure to clastogenic concentrations of LC. However, clastogenesis was not observed after exposure to LG, even when intracellular Pb concentrations reached 13,347microM, indicating that intracellular Pb levels did not reach clastogenic levels in WTHBF-6 cells after LC treatment. By contrast, SC was clastogenic damaging 16 and 44% of metaphase cells at intracellular Cr doses of 312 and 1262microM respectively, which was comparable to the clastogenesis observed after LC treatment. LC damaged 10, 27 and 37% of metaphases at intracellular Cr doses of 288, 926 and 1644microM, respectively. These data indicate that with respect to LC-induced clastogenicity, Cr and not Pb is the proximate clastogenic species in human lung cells.
机译:六价铬(Cr(VI))是一种公认​​的人类肺致癌物,具有潜在的广泛暴露范围。可溶性是Cr(VI)致癌性的关键因素,水不溶性或“微粒”化合物是更有效的致癌物。研究表明,组成离子是造成其致胶化作用的原因,但不确定铬(Cr),铅(Pb)或两者的某种组合是否会造成致胶化作用。因此,我们在WTHBF-6人肺细胞中比较了铬酸铅(LC)与可溶性铬酸钠(SC)和谷氨酸铅(LG)的致裂解性。我们发现1436microM是暴露于杀灭性LC浓度后的最大细胞内Pb水平。然而,即使暴露于细胞内的Pb浓度达到13,347microM,也未观察到发生LG分裂的现象,这表明LC处理后WTHBF-6细胞中的细胞内Pb并未达到分裂的水平。相比之下,在细胞内Cr剂量分别为312和1262microM时,SC发生了致裂性破坏16%和44%的中期细胞,这与LC处理后观察到的致裂性相当。 LC在288、926和1644microM的细胞内Cr剂量下分别破坏了10%,27%和37%的中期。这些数据表明,就LC诱导的致分裂性而言,Cr(而非Pb)是人肺细胞中最接近的致分裂物种。

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