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首页> 外文期刊>Antioxidants and redox signalling >Thiol-Based Redox Switches in Eukaryotic Proteins
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Thiol-Based Redox Switches in Eukaryotic Proteins

机译:真核蛋白中基于硫醇的氧化还原开关

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For many years, oxidative thiol modifications in cytosolic proteins were largely disregarded as in vitro artifacts, and considered unlikely to play significant roles within the reducing environment of the cell. Recent developments in in vivo thiol trapping technology combined with mass spectrometric analysis have now provided convincing evidence that thiol-based redox switches are used as molecular tools in many proteins to regulate their activity in response to reactive oxygen and nitrogen species. Reversible oxidative thiol modifications have been found to modulate the function of proteins involved in many different pathways, starting from gene transcription, translation and protein folding, to metabolism, signal transduction, and ultimately apoptosis. This review will focus on three well-characterized eukaryotic proteins that use thiol-based redox switches to influence gene transcription, metabolism, and signal transduction. The transcription factor Yaplp is a good illustration of how oxidative modifications affect the function of a protein without changing its activity. We use glyeraldehyde-3-phosphate dehydrogenase to demonstrate how thiol modification of an active site cysteine re-routes metabolic pathways and converts a metabolic enzyme into a pro-apoptotic factor. Finally, we introduce the redox-sensitive protein tyrosine phosphatase PTP1B to illustrate that reversibility is one of the fundamental aspects of redox-regulation.
机译:多年以来,胞质蛋白中的氧化硫醇修饰在很大程度上被忽略为体外人工产物,并且被认为不太可能在细胞的还原环境中发挥重要作用。体内硫醇捕集技术与质谱分析相结合的最新进展现已提供令人信服的证据,表明基于硫醇的氧化还原开关已被用作许多蛋白质的分子工具,以调节其对活性氧和氮物种的响应。已发现可逆的氧化硫醇修饰可调节参与许多不同途径的蛋白质的功能,这些途径从基因转录,翻译和蛋白质折叠开始,到代谢,信号转导,最后到细胞凋亡。这篇综述将集中在三个特征明确的真核蛋白质上,这些蛋白质使用基于硫醇的氧化还原开关来影响基因转录,代谢和信号转导。转录因子Yaplp很好地说明了氧化修饰如何影响蛋白质的功能而不改变其活性。我们使用3-磷酸甘油醛脱氢酶来证明活性位点半胱氨酸的巯基修饰如何重新路由代谢途径并将代谢酶转化为促凋亡因子。最后,我们介绍了氧化还原敏感蛋白酪氨酸磷酸酶PTP1B,以说明可逆性是氧化还原调节的基本方面之一。

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