内质网蛋白57和塔帕辛对主要组织相容性复合体I类分子肽接受性的氧化还原调节

Redox regulation of peptide receptivity of major histocompatibility complex class I molecules by ERp57 and tapasin.

作者信息

Kienast Alexandra, Preuss Marc, Winkler Monique, Dick Tobias P

机构信息

Redox Regulation Research Group, German Cancer Research Center, D-69120 Heidelberg, Germany.

出版信息

Nat Immunol. 2007 Aug;8(8):864-72. doi: 10.1038/ni1483. Epub 2007 Jul 1.

DOI:10.1038/ni1483

PMID:17603488

Abstract

The function of the oxidoreductase ERp57 in the major histocompatibility complex (MHC) class I peptide-loading complex has remained elusive. Here we show that in the absence of tapasin, the alpha2 disulfide bond in the MHC class I peptide-binding groove was rapidly reduced. Covalent sequestration of ERp57 by tapasin was needed to protect the alpha2 disulfide bond against reduction and thus to maintain the binding groove in a peptide-receptive state. Allelic variations in MHC class I tapasin dependency reflected their susceptibility to reduction of the alpha2 disulfide bond. In the absence of sequestration, ERp57 acted directly on the alpha2 disulfide bond. Our work provides insight into how the immune system customizes 'quality control' in the endoplasmic reticulum to fit the needs of antigen presentation.

摘要

氧化还原酶ERp57在主要组织相容性复合体（MHC）I类肽装载复合体中的功能一直难以捉摸。在此我们表明，在没有塔帕辛的情况下，MHC I类肽结合槽中的α2二硫键会迅速还原。塔帕辛对ERp57的共价隔离是保护α2二硫键不被还原从而使结合槽维持在肽接受状态所必需的。MHC I类对塔帕辛的依赖性的等位基因变异反映了它们对α2二硫键还原的敏感性。在没有隔离的情况下，ERp57直接作用于α2二硫键。我们的工作为免疫系统如何在内质网中定制“质量控制”以满足抗原呈递的需求提供了见解。

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内质网蛋白57和塔帕辛对主要组织相容性复合体I类分子肽接受性的氧化还原调节

Redox regulation of peptide receptivity of major histocompatibility complex class I molecules by ERp57 and tapasin.

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