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抗原加工途径及II类主要组织相容性复合体肽捕获的重建

Reconstruction of a pathway of antigen processing and class II MHC peptide capture.

作者信息

Moss Catherine X, Tree Timothy I, Watts Colin

机构信息

Division of Cell Biology & Immunology, School of Life Sciences, University of Dundee, Dundee, UK.

出版信息

EMBO J. 2007 Apr 18;26(8):2137-47. doi: 10.1038/sj.emboj.7601660. Epub 2007 Mar 29.

Abstract

Endocytosed antigens are proteolytically processed and small amounts of peptides captured by class II MHC molecules. The details of antigen proteolysis, peptide capture and how destruction of T-cell epitopes is avoided are incompletely understood. Using the tetanus toxin antigen, we show that the introduction of 3-6 cleavage sites is sufficient to trigger a partially unfolded conformation able to bind to class II MHC molecules. The known locations of T-cell epitopes and protease cleavage sites predict that large domains of processed antigen (8-35 kDa) are captured under these conditions. Remarkably, when antigen is bound to the B-cell antigen receptor (BCR), processing can trigger a concerted 'hand-over' reaction whereby BCR-associated processed antigen is captured by neighbouring class II MHC molecules. Early capture of minimally processed antigen and confinement of the processing and class II MHC loading reaction to the membrane plane may improve the likelihood of T-cell epitope survival in the class II MHC pathway and may help explain the reciprocal relationships observed between B- and T-cell epitopes in many protein antigens and autoantigens.

摘要

内吞的抗原会被蛋白水解处理,少量肽段被II类主要组织相容性复合体(MHC)分子捕获。目前对抗原蛋白水解、肽段捕获以及如何避免T细胞表位被破坏的细节了解尚不完全。利用破伤风毒素抗原,我们发现引入3至6个切割位点足以触发一种能与II类MHC分子结合的部分解折叠构象。已知的T细胞表位和蛋白酶切割位点的位置预测,在这些条件下,加工后的抗原的大片段(8至35 kDa)会被捕获。值得注意的是,当抗原与B细胞抗原受体(BCR)结合时,加工过程可触发协同的“交接”反应,即与BCR相关的加工抗原被邻近的II类MHC分子捕获。对最低限度加工抗原的早期捕获以及将加工和II类MHC装载反应限制在膜平面内,可能会提高T细胞表位在II类MHC途径中存活的可能性,并且可能有助于解释在许多蛋白质抗原和自身抗原中观察到的B细胞和T细胞表位之间的相互关系。

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