首页> 外文期刊>Journal of biological inorganic chemistry: JBIC: a publication of the Society of Biological Inorganic Chemistry >Time-dependent uptake, distribution and biotransformation of chromium(VI) in individual and bulk human lung cells: application of synchrotron radiation techniques
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Time-dependent uptake, distribution and biotransformation of chromium(VI) in individual and bulk human lung cells: application of synchrotron radiation techniques

机译:单个和大量人类肺细胞中铬(VI)的时间依赖性吸收,分布和生物转化:同步辐射技术的应用

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摘要

Chromium( VI) is a human carcinogen, primarily affecting the respiratory tract probably via active transport into cells, followed by the reduction to Cr(III) with the formation of DNA-damaging intermediates. Distribution of Cr and endogenous elements within A549 human lung adenocarcinoma epithelial cells, following treatment with Cr( VI) ( 100 mu M, 20 min or 4 h) were studied by synchrotron-radiation-induced X-ray emission (SRIXE) of single freeze-dried cells. After the 20-min treatment, Cr was confined to a small area of the cytoplasm and strongly co-localized with S, Cl, K, and Ca. After the 4-h treatment, Cr was distributed throughout the cell, with higher concentrations in the nucleus and the cytoplasmic membrane. This time-dependence corresponded to similar to 100% or 0% clonogenic survival of the cells following the 20-min or 4-h treatments, respectively, and could potentially be explained by a new cellular protective mechanism. Such processes may also be important in reducing the potential hazards of Cr( III) dietary supplements, for which there is emerging evidence that they exert their anti-diabetic effects via biological oxidation to Cr(VI). The predominance of Cr(III) was confirmed by micro-XANES spectroscopy of intracellular Cr hotspots. X-ray absorption spectroscopy (XANES and EXAFS, using freeze-dried cells after the 0 - 4-h treatments) was used to gain insight into the chemical structures of Cr( III) complexes formed during the intracellular reduction of Cr( VI). The polynuclear nature of such complexes ( probably with a combination of carboxylato and hydroxo bridging groups and O-donor atoms of small peptides or proteins) was established by XAFS data analyses.
机译:铬(VI)是一种人类致癌物,可能主要通过主动转运到细胞中来影响呼吸道,然后还原为Cr(III)并形成破坏DNA的中间体。通过同步冷冻辐射诱导的单次冷冻X射线发射(SRIXE)研究了Cr(VI)(100μM,20 min或4 h)处理后A549人肺腺癌上皮细胞中Cr和内源性元素的分布干细胞。 20分钟的处理后,Cr被限制在细胞质的一小部分,并与S,Cl,K和Ca强烈共定位。经过4小时的处理后,Cr分布在整个细胞中,并且在细胞核和细胞质膜中的含量更高。这种时间依赖性分别相当于在20分钟或4小时处理后,细胞的克隆形成存活率接近100%或0%,并且可能通过新的细胞保护机制来解释。此类过程对于减少Cr(III)膳食补充剂的潜在危害也可能很重要,为此,越来越多的证据表明它们通过生物氧化Cr(VI)发挥抗糖尿病作用。 Cr(III)的优势已通过细胞内Cr热点的微XANES光谱法得以证实。 X射线吸收光谱法(XANES和EXAFS,在0-4小时处理后使用冻干细胞)用于深入了解在细胞内Cr(VI)还原过程中形成的Cr(III)配合物的化学结构。通过XAFS数据分析确定了此类复合物的多核性质(可能与羧基和羟基桥接基团以及小肽或蛋白质的O供体原子的组合)。

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