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Identification and metabolism of selenocysteine-glutathione selenenyl sulfide (CySeSG) in small intestine of mice orally exposed to selenocystine.

作者信息

Hasegawa T, Okuno T, Nakamuro K, Sayato Y

机构信息

Division of Environmental Health, Faculty of Pharmaceutical Sciences, Setsunan University, Osaka, Japan.

出版信息

Arch Toxicol. 1996;71(1-2):39-44. doi: 10.1007/s002040050356.

DOI:10.1007/s002040050356
PMID:9010584
Abstract

This investigation was carried out to elucidate the chemical form of selenium-containing metabolite in small intestine of ICR male mice orally administered selenocystine (CySeSeCy). The metabolite in intestinal cytosol of mice treated with CySeSeCy (50 mg/kg) was identified as selenocysteine-glutathione selenenyl sulfide (CySeSG) by high performance liquid chromatography using a gel filtration and reversed phase column. Hydrogen selenide formation was caused as a result of the anaerobic reaction between the CySeSG and liver cytosol containing selenocysteine beta-lyase, which specifically acts on selenocysteine (CySeH). Effects of GSH or glutathione reductase on hydrogen selenide formation from CyseSG reacted with the liver cytosol were examined. The CySeSG was nonenzymatically reduced to CySeH by excess GSH in the liver cytosol. It was also recognized that CySeSG was enzymatically reduced to CySeH by glutathione reductase in the presence of NADPH. These results indicate that the chemical form of this metabolite is CySeSG, which has a molecular weight of 473, the CySeSG is then reduced by excess GSH and/or glutathione reductase yielding CySeH, which is decomposed by selenocysteine beta-lyase to hydrogen selenide. CySeSG may be a stable precursor of hydrogen selenide in animals.

摘要

相似文献

1
Identification and metabolism of selenocysteine-glutathione selenenyl sulfide (CySeSG) in small intestine of mice orally exposed to selenocystine.
Arch Toxicol. 1996;71(1-2):39-44. doi: 10.1007/s002040050356.
2
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[Selenium methylation and toxicity mechanism of selenocystine].[硒代胱氨酸的硒甲基化及毒性机制]
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Distribution and chemical form of selenium in mice after administration of selenocystine.
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6
Human thioredoxin reductase directly reduces lipid hydroperoxides by NADPH and selenocystine strongly stimulates the reaction via catalytically generated selenols.人硫氧还蛋白还原酶通过NADPH直接还原脂质氢过氧化物,而硒代胱氨酸通过催化生成的硒醇强烈刺激该反应。
J Biol Chem. 1995 May 19;270(20):11761-4. doi: 10.1074/jbc.270.20.11761.
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Synthesis of [75Se]trimethylselenonium iodide from [75Se]selenocystine.由[75Se]硒代胱氨酸合成[75Se]碘化三甲基硒鎓。
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Selenocysteine beta-lyase and methylselenol demethylase in the metabolism of Se-methylated selenocompounds into selenide.硒代半胱氨酸β-裂解酶和甲基硒醇脱甲基酶在甲基化硒化合物代谢为硒化物的过程中发挥作用。
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