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生物学中的硒:事实与医学展望。

Selenium in biology: facts and medical perspectives.

作者信息

Köhrl J, Brigelius-Flohé R, Böck A, Gärtner R, Meyer O, Flohé L

机构信息

University of Würzburg, Division Molecular Internal Medicine, Medizinische Poliklinik, Germany.

出版信息

Biol Chem. 2000 Sep-Oct;381(9-10):849-64. doi: 10.1515/BC.2000.107.

Abstract

Several decades after the discovery of selenium as an essential trace element in vertebrates approximately 20 eukaryotic and more than 15 prokaryotic selenoproteins containing the 21st proteinogenic amino acid, selenocysteine, have been identified, partially characterized or cloned from several species. Many of these proteins are involved in redox reactions with selenocysteine acting as an essential component of the catalytic cycle. Enzyme activities have been assigned to the glutathione peroxidase family, to the thioredoxin reductases, which were recently identified as selenoproteins, to the iodothyronine deiodinases, which metabolize thyroid hormones, and to the selenophosphate synthetase 2, which is involved in selenoprotein biosynthesis. Prokaryotic selenoproteins catalyze redox reactions and formation of selenoethers in (stress-induced) metabolism and energy production of E. coli, of the clostridial cluster XI and of other prokaryotes. Apart from the specific and complex biosynthesis of selenocysteine, selenium also reversibly binds to proteins, is incorporated into selenomethionine in bacteria, yeast and higher plants, or posttranslationally modifies a catalytically essential cysteine residue of CO dehydrogenase. Expression of individual eukaryotic selenoproteins exhibits high tissue specificity, depends on selenium availability, in some cases is regulated by hormones, and if impaired contributes to several pathological conditions. Disturbance of selenoprotein expression or function is associated with deficiency syndromes (Keshan and Kashin-Beck disease), might contribute to tumorigenesis and atherosclerosis, is altered in several bacterial and viral infections, and leads to infertility in male rodents.

摘要

在硒被发现是脊椎动物必需的微量元素几十年后,已从多个物种中鉴定、部分表征或克隆出约20种真核和15种以上原核含第21种蛋白质氨基酸硒代半胱氨酸的硒蛋白。这些蛋白质中的许多都参与氧化还原反应,硒代半胱氨酸作为催化循环的必需成分。已将酶活性赋予谷胱甘肽过氧化物酶家族、最近被鉴定为硒蛋白的硫氧还蛋白还原酶、代谢甲状腺激素的碘甲状腺原氨酸脱碘酶以及参与硒蛋白生物合成的硒磷酸合成酶2。原核硒蛋白在大肠杆菌、梭菌属XI簇和其他原核生物的(应激诱导的)代谢和能量产生中催化氧化还原反应和硒醚的形成。除了硒代半胱氨酸特异而复杂的生物合成外,硒还可逆地与蛋白质结合,在细菌、酵母和高等植物中掺入硒代蛋氨酸,或在翻译后修饰一氧化碳脱氢酶的催化必需半胱氨酸残基。单个真核硒蛋白的表达表现出高度的组织特异性,取决于硒的可利用性,在某些情况下受激素调节,若受损则会导致多种病理状况。硒蛋白表达或功能的紊乱与缺乏综合征(克山病和大骨节病)相关,可能促成肿瘤发生和动脉粥样硬化,在几种细菌和病毒感染中发生改变,并导致雄性啮齿动物不育。

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