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首页> 外文期刊>Antioxidants and redox signalling >Redox regulation of protein tyrosine phosphatases: structural and chemical aspects.
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Redox regulation of protein tyrosine phosphatases: structural and chemical aspects.

机译:蛋白质酪氨酸磷酸酶的氧化还原调节:结构和化学方面。

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Protein tyrosine phosphatases (PTPs) are important targets of the H(2)O(2) that is produced during mammalian signal transduction. H(2)O(2)-mediated inactivation of PTPs also may be important in various pathophysiological conditions involving oxidative stress. Here we review the chemical and structural biology of redox-regulated PTPs. Reactions of H(2)O(2) with PTPs convert the catalytic cysteine thiol to a sulfenic acid. In PTPs, the initially generated sulfenic acid residues have the potential to undergo secondary reactions with a neighboring amide nitrogen or cysteine thiol residue to yield a sulfenyl amide or disulfide, respectively. The chemical mechanisms by which formation of sulfenyl amide and disulfide linkages can protect the catalytic cysteine residue against irreversible overoxidation to sulfinic and sulfonic oxidation states are described. Due to the propensity for back-door and distal cysteine residues to engage with the active-site cysteine after oxidative inactivation, differences in the structures of the oxidatively inactivated PTPs may stem, to a large degree, from differences in the number and location of cysteine residues surrounding the active site of the enzymes. PTPs with key cysteine residues in structurally similar locations may be expected to share similar mechanisms of oxidative inactivation.
机译:蛋白酪氨酸磷酸酶(PTPs)是哺乳动物信号转导过程中产生的H(2)O(2)的重要目标。 H(2)O(2)介导的PTP失活在涉及氧化应激的各种病理生理状况中也可能很重要。在这里,我们审查氧化还原调节的PTPs的化学和结构生物学。 H(2)O(2)与PTP的反应将催化的半胱氨酸硫醇转化为亚磺酸。在PTP中,最初生成的亚磺酸残基有可能与邻近的酰胺氮或半胱氨酸硫醇残基发生二级反应,分别生成亚磺酰胺或二硫化物。描述了形成亚磺酰胺键和二硫键可以保护催化的半胱氨酸残基免受不可逆的过氧化成亚磺酸和磺酸氧化态的化学机理。由于氧化灭活后后半部和远端半胱氨酸残基倾向于与活性位点的半胱氨酸结合,氧化灭活的PTP的结构差异在很大程度上可能是由于半胱氨酸的数量和位置的差异酶活性位点周围的残基。在结构上相似位置具有关键半胱氨酸残基的PTP有望共享相似的氧化失活机理。

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