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作为MHC II类分子内吞抗原捕获底物的大蛋白质片段。

Large protein fragments as substrates for endocytic antigen capture by MHC class II molecules.

作者信息

Castellino F, Zappacosta F, Coligan J E, Germain R N

机构信息

Lymphocyte Biology Section, Laboratory of Immunology, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

J Immunol. 1998 Oct 15;161(8):4048-57.

PMID:9780175
Abstract

Although the binding sites of MHC class II molecules can accommodate longer ligands, peptides of 15 to 20 residues are the primary form of processed Ag recovered from class II dimers isolated from living cells. These peptides are derived from intact Ags by proteolysis in endocytic organelles, where binding to class II dimers also occurs. Whether generation of these short peptides typically precedes association with class II molecules, or whether class II molecules initially bind to unfolded proteins or large protein fragments, followed by degradation of the unprotected regions, remains unknown. Here we report the identification of an SDS-stable, long-lived, 120-kDa complex composed of two class II dimers bound to a common large Ag fragment. This complex is produced within the endocytic pathway from newly synthesized MHC class II molecules following exposure of the cells to exogenous hen egg lysozyme. These data suggest that a major pathway of Ag processing involves the initial binding of class II heterodimers to large protein substrates upon exposure of regions with suitable motifs, followed by cleavage and/or trimming of the exposed protein around this bound region. This sequence of events during Ag processing may provide a partial molecular explanation for the immunodominance of certain determinants in protein Ags.

摘要

尽管MHC II类分子的结合位点能够容纳更长的配体,但从活细胞分离的II类二聚体中回收的已加工抗原的主要形式是15至20个残基的肽段。这些肽段是通过内吞细胞器中的蛋白水解作用从完整抗原衍生而来的,在那里它们也与II类二聚体结合。这些短肽的产生通常是先于与II类分子结合,还是II类分子最初先结合未折叠的蛋白质或大的蛋白质片段,随后未受保护区域发生降解,目前尚不清楚。在此,我们报告鉴定出一种SDS稳定、寿命长的120 kDa复合物,它由两个与共同的大抗原片段结合的II类二聚体组成。这种复合物是在细胞暴露于外源性鸡卵溶菌酶后,由新合成的MHC II类分子在内吞途径中产生的。这些数据表明,抗原加工的主要途径涉及II类异二聚体在暴露有合适基序的区域后,先与大的蛋白质底物结合,随后在该结合区域周围对暴露的蛋白质进行切割和/或修剪。抗原加工过程中的这一系列事件可能为蛋白质抗原中某些决定簇的免疫显性提供部分分子解释。

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