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首页> 外文期刊>The Journal of biological chemistry >Different Interaction Modes for Protein-disulfide Isomerase (PDI) as an Efficient Regulator and a Specific Substrate of Endoplasmic Reticulum Oxidoreductin-1α (Ero1α)
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Different Interaction Modes for Protein-disulfide Isomerase (PDI) as an Efficient Regulator and a Specific Substrate of Endoplasmic Reticulum Oxidoreductin-1α (Ero1α)

机译:蛋白质二硫化物异构酶(PDI)作为高效调节剂的不同相互作用模式和内质网氧化素-1α(ERO1α)的特定基材

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摘要

Protein-disulfide isomerase (PDI) and sulfhydryl oxidase endoplasmic reticulum oxidoreductin-1α (Ero1α) constitute the pivotal pathway for oxidative protein folding in the mammalian endoplasmic reticulum (ER). Ero1α oxidizes PDI to introduce disulfides into substrates, and PDI can feedback-regulate Ero1α activity. Here, we show the regulatory disulfide of Ero1α responds to the redox fluctuation in ER very sensitively, relying on the availability of redox active PDI. The regulation of Ero1α is rapidly facilitated by either a or a′ catalytic domain of PDI, independent of the substrate binding domain. On the other hand, activated Ero1α specifically binds to PDI via hydrophobic interactions and preferentially catalyzes the oxidation of domain a′. This asymmetry ensures PDI to function simultaneously as an oxidoreductase and an isomerase. In addition, several PDI family members are also characterized to be potent regulators of Ero1α. The novel modes for PDI as a competent regulator and a specific substrate of Ero1α govern efficient and faithful oxidative protein folding and maintain the ER redox homeostasis.
机译:蛋白质 - 二硫化物异构酶(PDI)和巯基氧化酶内质网氧化酰胺-1α(ERO1α)构成哺乳动物内质网(ER)中的氧化蛋白折叠的关键途径。 ERO1α将PDI氧化以将二硫化物引入底物中,并且PDI可以反馈 - 调节ERO1α活性。在这里,我们展示了ERO1α的调节性二硫化物非常敏感地响应氧化还原波动,依赖于氧化还原活性PDI的可用性。通过PDI的A或“催化结构域”迅速促进ERO1α的调节,与底物结合结构域无关。另一方面,活化的ERO1α通过疏水相互作用特异性结合PDI,优先催化结构域A'的氧化。该不对称性确保PDI同时用作氧化还原酶和异构酶。此外,几个PDI家族成员的特征还表明是ERO1α的有效调节因子。 PDI作为称重稳压剂的新型模式和ERO1α的特定基材治理有效和忠实的氧化蛋白折叠,维持ER氧化还原稳态。

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