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哺乳动物细胞中铬(VI)生物转化的X射线吸收和电子顺磁共振光谱研究。铬调蛋白是分离方法的人为产物吗?

X-ray absorption and EPR spectroscopic studies of the biotransformations of chromium(VI) in mammalian cells. Is chromodulin an artifact of isolation methods?

作者信息

Levina Aviva, Harris Hugh H, Lay Peter A

机构信息

Centre for Heavy Metals Research, School of Chemistry, The University of Sydney, NSW 2006, Australia.

出版信息

J Am Chem Soc. 2007 Feb 7;129(5):1065-75. doi: 10.1021/ja063792r.

Abstract

Very different biological activities are usually ascribed to Cr(VI) (a toxin and carcinogen) and Cr(III) (an antidiabetic agent), although recent evidence suggests that both these types of actions are likely to arise from cellular uptake of varying concentrations of Cr(VI). The first systematic study of XANES spectra of Cr(III) complexes formed in Cr(VI)-treated mammalian cells (A549, HepG2, V79, and C2C12 cell lines), and in subcellular fractions of A549 cells, has been performed using a library of XANES spectra of model Cr(III) complexes. The results of multiple linear regression analyses of XANES spectra, in combination with multiple-scattering fits of XAFS spectra, indicate that Cr(III) formed in Cr(VI)-treated cells is most likely to bind to carboxylato, amine, and imidazole residues of amino acids, and to a lesser extent to hydroxo or aqua ligands. A combination of XANES and EPR spectroscopic data for Cr(VI)-treated cells indicates that the main component of Cr(III) formed in such cells is bound to high-molecular-mass ligands (>30 kDa, probably proteins), but significant redistribution of Cr(III) occurs during the cell lysis, which leads to the formation of a low-molecular-mass (<30 kDa) Cr(III)-containing fraction. The spectroscopic (XANES, XAFS, and EPR) properties of this fraction were strikingly similar to those of the purported natural Cr(III)-containing factor, chromodulin, that was reported to be isolated from the reaction of Cr(VI) with liver. These data support the hypothesis that a chromodulin-like species, which is formed from such a reaction, is an artifact of the reported isolation procedure.

摘要

通常认为六价铬(一种毒素和致癌物)和三价铬(一种抗糖尿病剂)具有截然不同的生物活性,尽管最近的证据表明,这两种作用可能都源于细胞对不同浓度六价铬的摄取。利用一系列模型三价铬配合物的X射线吸收近边结构(XANES)光谱库,首次对六价铬处理的哺乳动物细胞(A549、HepG2、V79和C2C12细胞系)以及A549细胞亚细胞组分中形成的三价铬配合物的XANES光谱进行了系统研究。XANES光谱的多元线性回归分析结果,结合X射线吸收精细结构(XAFS)光谱的多重散射拟合,表明六价铬处理的细胞中形成的三价铬最有可能与氨基酸的羧基、胺基和咪唑残基结合,在较小程度上与羟基或水配体结合。六价铬处理细胞的XANES和电子顺磁共振(EPR)光谱数据表明,此类细胞中形成的三价铬的主要成分与高分子质量配体(>30 kDa,可能是蛋白质)结合,但在细胞裂解过程中三价铬会发生显著重新分布,导致形成低分子质量(<30 kDa)的含三价铬组分。该组分的光谱(XANES、XAFS和EPR)性质与据称从六价铬与肝脏反应中分离出的天然含三价铬因子铬调素的性质惊人地相似。这些数据支持了这样一种假设,即由这种反应形成的类铬调素物质是所报道的分离过程产生的假象。

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