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首页> 外文期刊>Metallomics. integrated biometal science >Selenium-mediated arsenic excretion in mammals: a synchrotron-based study of whole-body distribution and tissue-specific chemistry
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Selenium-mediated arsenic excretion in mammals: a synchrotron-based study of whole-body distribution and tissue-specific chemistry

机译:硒介导的哺乳动物中的砷排泄:基于同步的全身分布和组织特异性化学研究

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Arsenicosis, a syndrome caused by ingestion of arsenic contaminated drinking water, currently affects millions of people in South-East Asia and elsewhere. Previous animal studies revealed that the toxicity of arsenite essentially can be abolished if selenium is co-administered as selenite. Although subsequent studies have provided some insight into the biomolecular basis of this striking antagonism, many details of the biochemical pathways that ultimately result in the detoxification and excretion of arsenic using selenium supplements have yet to be thoroughly studied. To this end and in conjunction with the recent Phase III clinical trial "Selenium in the Treatment of Arsenic Toxicity and Cancers'', we have applied synchrotron X-ray techniques to elucidate the mechanisms of this arsenic-selenium antagonism at the tissue and organ levels using an animal model. X-ray fluorescence imaging (XFI) of cryo-dried whole-body sections of laboratory hamsters that had been injected with arsenite, selenite, or both chemical species, provided insight into the distribution of both metalloids 30 minutes after treatment. Co-treated animals showed strong co-localization of arsenic and selenium in the liver, gall bladder and small intestine. X-ray absorption spectroscopy (XAS) of freshly frozen organs of co-treated animals revealed the presence in liver tissues of the seleno bis-(S-glutathionyl) arsinium ion, which was rapidly excreted via bile into the intestinal tract. These results firmly support the previously postulated hepatobiliary excretion of the seleno bis-(S-glutathionyl) arsinium ion by providing the first data pertaining to organs of whole animals.
机译:砷菌,一种由摄入砷污染饮用水引起的综合征,目前影响了数百万的东南亚和其他地方。以前的动物研究表明,如果硒作为硒矿石共同施用,则砷的毒性基本上可以废除。虽然随后的研究已经提供了对这种引人注目的拮抗作用的生物分子基础的洞察,但是最终导致使用硒补充剂的砷的解毒和排泄的生化途径的许多细节。为此,结合近期III期临床试验“硒治疗砷毒性和癌症”,我们应用同步X射线技术,以阐明在组织和器官水平的砷 - 硒拮抗作用的机制使用动物模型。用砷酸盐,硒矿或两种化学物质注射的实验室仓鼠的冷冻干燥全身部分的X射线荧光成像(XFI)提供了在处理后30分钟内容的洞察两种金属体的分布。共同处理的动物显示肝脏,胆囊和小肠中砷和硒的强烈共定。X射线吸收光谱(XAs)的共同处理动物的新冷冻器官揭示了Seleno的肝组织中的存在双(S-谷胱甘肽)亚胆管离子,将通过胆汁迅速排出到肠道中。这些结果牢固地支持先前假期的肝胆胆醌排泄的Seleno BIS-( S-谷胱甘肽通过提供与整个动物的器官有关的第一数据。

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