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首页> 外文期刊>Journal of Molecular Biology >Molecular Mechanisms of Glutaredoxin Enzymes: Versatile Hubs for Thiol-Disulfide Exchange between Protein Thiols and Glutathione
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Molecular Mechanisms of Glutaredoxin Enzymes: Versatile Hubs for Thiol-Disulfide Exchange between Protein Thiols and Glutathione

机译:戊二糖胺酶的分子机制:蛋白质硫醇和谷胱甘肽之间的硫醇二硫化物交换的通用枢轴

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摘要

The tripeptide glutathione (GSH) and its oxidized form glutathione disulfide (GSSG) constitute a key redox couple in cells. In particular, they partner protein thiols in reversible thiol-disulfide exchange reactions that act as switches in cell signaling and redox homeostasis. Disruption of these processes may impair cellular redox signal transduction and induce redox misbalances that are linked directly to aging processes and to a range of pathological conditions including cancer, cardiovascular diseases and neurological disorders. Glutaredoxins are a class of GSH-dependent oxidoreductase enzymes that specifically catalyze reversible thiol-disulfide exchange reactions between protein thiols and the abundant thiol pool GSSG/GSH. They protect protein thiols from irreversible oxidation, regulate their activities under a variety of cellular conditions and are key players in cell signaling and redox homeostasis. On the other hand, they may also function as metal-binding proteins with a possible role in the cellular homeostasis and metabolism of essential metals copper and iron. However, the molecular basis and underlying mechanisms of glutaredoxin action remain elusive in many situations. This review focuses specifically on these aspects in the context of recent developments that illuminate some of these uncertainties. (C) 2018 Elsevier Ltd. All rights reserved.
机译:三肽谷胱甘肽(GSH)及其氧化形式的谷胱甘肽二硫化物(GSSG)构成细胞中的关键氧化还原耦合。特别是,它们在可逆的硫醇二硫化物交换反应中伴侣蛋白硫醇,其充当细胞信号传导和氧化还原稳态的开关。这些过程的破坏可能会损害细胞氧化还原信号转导,并诱导直接与老化过程连接的氧化还原误操作以及一系列病理条件,包括癌症,心血管疾病和神经系统障碍。戊二酮是一类GSH依赖性氧化酶酶,其特异性地催化蛋白质硫醇和丰富的硫醇库GSSG / GSH之间的可逆硫醇二硫化物交换反应。它们保护蛋白质硫醇免受不可逆氧化,调节它们在各种细胞条件下的活性,并且是细胞信号传导和氧化还原稳态的关键参与者。另一方面,它们还可以用作金属结合蛋白质,其在细胞稳态和必需金属铜和铁的代谢中具有可能作用。然而,在许多情况下,谷氨酸毒素作用的分子基础和潜在机制仍然难以捉摸。本综述专注于近期发展的这些方面,以照亮其中一些不确定性。 (c)2018年elestvier有限公司保留所有权利。

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