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脱氢抗坏血酸在二硫键形成中的作用。

The role of dehydroascorbate in disulfide bond formation.

机构信息

Department of Biochemistry, University of Oulu, Oulu, Finland.

出版信息

Antioxid Redox Signal. 2010 Jan;12(1):15-25. doi: 10.1089/ars.2009.2674.

Abstract

Dehydroascorbate (DHA) is a higher oxidation state of ascorbate formed through its action as an intracellular antioxidant. The recycling of DHA back to ascorbate is thought to be catalyzed by a variety of enzymes, including protein disulfide isomerase (PDI), linking ascorbate metabolism to oxidative protein folding in the endoplasmic reticulum (ER). Here we examine the possible role of PDI as a dehydroascorbate reductase. We find the reaction too slow to be the major route for reduction of DHA in the ER, with a second-order rate constant for the reaction of reduced PDI with DHA of only 12.5 M(-1)s(-1). Rates of a similar order of magnitude were obtained for other thioredoxin-superfamily members. However, glutaredoxin was able to catalyze DHA reduction more rapidly through a monothiol mechanism. In addition, DHA can rapidly react with many other dithiol systems, including dithiols in unfolded or partially folded proteins in a PDI-independent manner, with second-order rate constants of up to 186 M(-1)s(-1). Furthermore, we identify borate as a potent inhibitor of catalyzed and noncatalyzed DHA reduction in vitro. This study both provides insights into the link between ascorbate metabolism and oxidative protein folding and suggests a novel link between ascorbate metabolism and borate toxicity.

摘要

脱氢抗坏血酸(DHA)是抗坏血酸作为细胞内抗氧化剂作用形成的更高氧化态。DHA 回收到抗坏血酸的循环被认为是由多种酶催化的,包括蛋白二硫键异构酶(PDI),将抗坏血酸代谢与内质网(ER)中的氧化蛋白折叠联系起来。在这里,我们研究了 PDI 作为脱氢抗坏血酸还原酶的可能作用。我们发现该反应速度太慢,不可能成为 ER 中 DHA 还原的主要途径,还原 PDI 与 DHA 的二级反应速率常数仅为 12.5 M(-1)s(-1)。对于其他硫氧还蛋白超家族成员,也得到了类似数量级的速率。然而,谷氧还蛋白能够通过单硫醇机制更快速地催化 DHA 还原。此外,DHA 可以快速与许多其他二硫键系统反应,包括 PDI 独立方式下未折叠或部分折叠蛋白质中的二硫键,其二级反应速率常数高达 186 M(-1)s(-1)。此外,我们确定硼酸在体外以催化和非催化方式抑制 DHA 还原。这项研究不仅深入了解了抗坏血酸代谢与氧化蛋白折叠之间的联系,还提出了抗坏血酸代谢与硼酸毒性之间的新联系。

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