首页> 美国卫生研究院文献>British Journal of Cancer >Cytotoxic and clastogenic effects of soluble and insoluble compounds containing hexavalent and trivalent chromium.
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Cytotoxic and clastogenic effects of soluble and insoluble compounds containing hexavalent and trivalent chromium.

机译:含有六价和三价铬的可溶性和不溶性化合物的细胞毒作用和破坏作用。

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摘要

Cr(III) and Cr(VI) compounds of varying solubilities have been tested in vitro for their ability to inhibit cell growth and nucleic acid and protein syntheses in BHK cells, to induce alterations in the mitotic cycle in HEp cells, and to increase the frequency of chromosomal aberrations and sister chromatid exchanges (SCE) in CHO cells. All Cr(VI) compounds, and particularly those containing soluble Cr(VI), such as potassium dichromate and zinc yellow, differentially inhibit macromolecular syntheses in BKH cells, that of DNA being always the most affected. Among Cr(III) compounds, which generally have very low cytotoxicity, chromite is particularly active, and inhibits cell growth and DNA synthesis even more than the poorly soluble Cr(VI) compounds. Preincubation in growth medium, with or without metabolizing cell cultures, solubilizes considerable amounts of Cr(VI) from zinc yellow and chromite, but significant amounts are also obtained from the most insoluble Cr(VI) pigments. When BHK cells are treated with such preincubated solutions, reduction of soluble Cr(VI) to Cr(III) by cell metabolites is seen with all Cr(VI) compounds, accompanied by decreased cytotoxicity. The same differences between Cr(VI) and Cr(III) compounds apply to the cytotoxic effects on mitosis of HEp cells and the clastogenic effects on CHO cells. The activity of chromite, the only Cr(III) pigment capable of significantly increasing the frequency of SCE, is due to contamination with soluble Cr(VI). In contrast to the very low cytotoxicity of Cr(III), much higher chromium levels are detected in the cells incubated with soluble Cr(III) than with the same concentrations of soluble Cr(VI). 50% and 75% of chromium accumulated in the cells during treatments with Cr(VI) and Cr(III) respectively remains firmly bound to the cells, even when they are incubated for up to 48 h in normal growth medium. Chromium accumulated in the cells after treatment with Cr(III) is most probably bound to the cell membrane, whereas some of the Cr(VI) is transported through the cell membrane and reduced in the cell nucleus. The results of the present investigation are in agreement with those obtained with the same Cr(VI) and Cr(III) compounds in mutagenicity assays in bacteria and carcinogenicity tests in rodents. A re-evaluation of the mechanisms of chromium carcinogenisis is proposed.
机译:已体外测试了不同溶解度的Cr(III)和Cr(VI)化合物在BHK细胞中抑制细胞生长以及核酸和蛋白质合成,诱导HEp细胞有丝分裂周期改变以及增加细胞凋亡的能力。 CHO细胞中的染色体畸变和姐妹染色单体交换(SCE)的频率。所有的Cr(VI)化合物,特别是那些含有可溶性Cr(VI)的化合物,例如重铬酸钾和锌黄,均会差异性地抑制BKH细胞中的大分子合成,而DNA总是最受影响。在通常具有极低细胞毒性的Cr(III)化合物中,亚铬酸盐特别活泼,甚至比难溶的Cr(VI)化合物更能抑制细胞生长和DNA合成。在有或没有代谢细胞培养物的情况下,在生长培养基中进行预温育可从锌黄和亚铬酸盐中溶解大量的Cr(VI),但是从最难溶的Cr(VI)颜料中也可获得大量的Cr(VI)。当用这种预温育的溶液处理BHK细胞时,所有的Cr(VI)化合物都可通过细胞代谢产物将可溶性Cr(VI)还原为Cr(III),同时降低了细胞毒性。 Cr(VI)和Cr(III)化合物之间的相同差异适用于对HEp细胞有丝分裂的细胞毒性作用和对CHO细胞的致胶化作用。亚铬酸盐的活性是唯一能显着增加SCE频率的Cr(III)颜料,这是由于可溶性Cr(VI)污染所致。与极低的Cr(III)细胞毒性相反,与相同浓度的可溶性Cr(VI)相比,在用可溶性Cr(III)孵育的细胞中检测到的铬水平高得多。即使在正常生长培养基中孵育长达48小时,在分别用Cr(VI)和Cr(III)处理期间,细胞中积累的50%和75%的铬仍与细胞牢固结合。 Cr(III)处理后,细胞中积累的铬最有可能与细胞膜结合,而某些Cr(VI)则通过细胞膜转运并在细胞核中还原。本研究的结果与在细菌的致突变性试验和啮齿类动物的致癌性试验中使用相同的Cr(VI)和Cr(III)化合物获得的结果一致。建议对致癌铬的机理进行重新评估。

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