首页> 美国卫生研究院文献>British Journal of Cancer >Cytotoxic and clastogenic effects of soluble chromium compounds on mammalian cell cultures.
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Cytotoxic and clastogenic effects of soluble chromium compounds on mammalian cell cultures.

机译:可溶性铬化合物对哺乳动物细胞培养物的细胞毒作用和破坏作用。

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摘要

The inhibition of cell growth, the reduction of cell survival and the induction of chromosome aberrations and of sister chromatid exchange (SCE) have been determined in cultured hamster cell lines (BHK and CHO) treated with 11 water-soluble compounds of hexavalent and trivalent chromium. All Cr6+ compounds inhibit growth of BHK cells and reduce survival of CHO cells to levels comparable to those obtained only after exposure to 100--1000 times higher Cr3+ concentrations. The cytotoxicity curves obtained with the different Cr6+ compounds are almost overlapping, whereas marked differences of activity are noticeable among Cr3+ compounds. Giant cells are obtained after exposure to Cr6+ and Cr3+ compounds, as shown by the rise of DNA and RNA per cell, and are due to the blockage of the cell cycle without sudden inhibition of macromolecular syntheses. Both Cr6+ and Cr3+ compounds are able to induce chromosome aberrations, whereas Cr3+ is absolutely incapable of inducing SCE, only Cr6+ being active. The frequency of chromosome aberrations is increased about 10-fold after exposure to 1.0 micrograms/ml Cr6+, whereas it is only doubled after treatment with up to 150 micrograms/ml Cr3+. On the other hand, in spite of the sensitivity of CHO cells to the induction of SCE by mitomycin C, the frequency of SCE hardly doubles after exposure to Cr6+ compounds. The present data confirm that Cr6+ compounds are characterized by a marked cytotoxicity and clastogenic action on mammalian cell cultures and show that Cr3+ compounds, though cytotoxic only at extremely high concentrations and not increasing the frequency of SCE, are not completely without cytogenetic effect, as they are able to induce chromosome aberrations.
机译:已在用11种六价和三价铬水溶性化合物处理的仓鼠细胞系(BHK和CHO)中确定了抑制细胞生长,降低细胞存活率以及诱导染色体畸变和姐妹染色单体交换(SCE)的作用。所有Cr6 +化合物均会抑制BHK细胞的生长并将CHO细胞的存活率降低至与暴露于较高Cr3 +浓度100--1000倍后获得的水平相当的水平。用不同的Cr6 +化合物获得的细胞毒性曲线几乎重叠,而Cr3 +化合物之间的活性差异明显。巨细胞是在暴露于Cr6 +和Cr3 +化合物后获得的,如每个细胞的DNA和RNA的增加所显示,这是由于细胞周期受阻而没有突然抑制大分子合成。 Cr6 +和Cr3 +化合物均能够诱导染色体畸变,而Cr3 +绝对不能诱导SCE,只有Cr6 +具有活性。暴露于1.0微克/毫升Cr6 +后,染色体畸变的频率增加了约10倍,而使用高达150微克/毫升Cr3 +处理后,染色体畸变的频率仅增加了一倍。另一方面,尽管CHO细胞对丝裂霉素C诱导SCE的敏感性,但暴露于Cr6 +化合物后,SCE的频率几乎不会翻倍。目前的数据证实了Cr6 +化合物的特征在于对哺乳动物细胞培养物具有明显的细胞毒性和致胶裂作用,并且表明Cr3 +化合物虽然仅在极高的浓度下才具有细胞毒性,并且不会增加SCE的发生频率,但它们并非完全没有细胞遗传作用,因为能够诱发染色体畸变。

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