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肽 - II类主要组织相容性复合体的构象异构体。

Conformational isomers of a peptide-class II major histocompatibility complex.

作者信息

Lovitch Scott B, Unanue Emil R

机构信息

Department of Pathology and Immunology, Washington University School of Medicine, St Louis, MO 63110, USA.

出版信息

Immunol Rev. 2005 Oct;207:293-313. doi: 10.1111/j.0105-2896.2005.00298.x.

Abstract

The relative plasticity of peptide binding to class II major histocompatibility complex (MHC) molecules permits formation of multiple conformational isomers by the same peptide and MHC molecule; such conformers are specifically recognized by distinct subsets of T cells. Here, we review current knowledge and recent advances in our understanding of peptide-class II MHC conformational isomerism and the mechanisms that generate distinct MHC-peptide conformers. We focus on our studies of two T-cell subsets, type A and B, which recognize distinct conformers of the dominant epitope of hen egg white lysozyme presented by I-A(k). These conformers form via different pathways and in distinct intracellular vesicles: the type A conformer forms in late endosomes upon processing of native protein, while the more flexible type B conformer forms in early endosomes and at the cell surface. In this process, H2-DM acts as a conformational editor, eliminating the type B conformer in late endosomes. Type B T cells constitute a significant component of the naïve T-cell repertoire; furthermore, self-reactive type B T cells escape negative selection and are present in abundance in the periphery. Ongoing studies should elucidate the role of type B T cells in immunity to pathogens and in autoimmune pathology.

摘要

肽与II类主要组织相容性复合体(MHC)分子结合的相对可塑性使得同一肽和MHC分子能够形成多种构象异构体;这些构象异构体可被不同的T细胞亚群特异性识别。在此,我们综述了目前关于肽-II类MHC构象异构现象以及产生不同MHC-肽构象异构体机制的认识和最新进展。我们重点介绍了对A、B两型T细胞亚群的研究,这两个亚群可识别由I-A(k)呈递的蛋清溶菌酶优势表位的不同构象异构体。这些构象异构体通过不同途径在不同的细胞内囊泡中形成:A型构象异构体在晚期内体中由天然蛋白加工形成,而更具灵活性的B型构象异构体则在早期内体和细胞表面形成。在此过程中,H2-DM充当构象编辑蛋白,在晚期内体中消除B型构象异构体。B型T细胞是初始T细胞库的重要组成部分;此外,自身反应性B型T细胞逃避阴性选择并大量存在于外周。正在进行的研究应能阐明B型T细胞在病原体免疫和自身免疫病理中的作用。

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