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应对主要组织相容性复合体I类肽库中完美性的丧失。

Coping with loss of perfection in the MHC class I peptide repertoire.

作者信息

Blanchard Nicolas, Shastri Nilabh

机构信息

Division of Immunology, Department of Molecular and Cell Biology, University of California, Berkeley, Berkeley, CA 94720-3200, USA.

出版信息

Curr Opin Immunol. 2008 Feb;20(1):82-8. doi: 10.1016/j.coi.2007.12.004.

Abstract

The MHC class I molecules present thousands of peptides (pMHC I) on the cell surface for immune surveillance by CD8 T cells. The pMHC I repertoire normally contains peptides of perfect length and sequences suitable for binding each MHC I. The peptides are made by first fragmenting cytoplasmic proteins. The fragments are then transported into the endoplasmic reticulum (ER), where they are trimmed to appropriate length by the ER aminopeptidase associated with antigen processing (ERAAP) to generate the final pMHC I. Here, we review studies on the role of ERAAP in generating pMHC I from endogenous or viral proteins and their ability to elicit CD8 T cell responses. The absence of ERAAP profoundly disrupts the pMHC I repertoire which can have major consequences on the immune responses to endogenous and viral antigens.

摘要

MHC I类分子在细胞表面呈递数千种肽段(pMHC I),以供CD8 T细胞进行免疫监视。正常情况下,pMHC I库包含长度完美且序列适合与每种MHC I结合的肽段。这些肽段首先通过切割细胞质蛋白产生。然后,这些片段被转运到内质网(ER)中,在那里它们被与抗原加工相关的内质网氨肽酶(ERAAP)修剪至合适长度,以生成最终的pMHC I。在此,我们综述了关于ERAAP在从内源性或病毒蛋白生成pMHC I中的作用及其引发CD8 T细胞反应能力的研究。ERAAP的缺失会严重破坏pMHC I库,这可能对内源性和病毒抗原的免疫反应产生重大影响。

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