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MHC II类分子介导的抗原呈递

Antigen presentation by MHC class II molecules.

作者信息

Weenink S M, Gautam A M

机构信息

Human Genetics Group, John Curtin School of Medical Research, Australian National University, Canberra, Australia.

出版信息

Immunol Cell Biol. 1997 Feb;75(1):69-81. doi: 10.1038/icb.1997.11.

DOI:10.1038/icb.1997.11
PMID:9046437
Abstract

The treamendous explosion in the field of MHC research in the last 5 years has significantly advanced our understanding of antigen processing pathways, particularly with regard to details of MHC class II-mediated antigen presentation. MHC class II molecules at the surface of antigen presenting cells present antigenic peptides to CD4+ T helper cells. However for effective cell surface antigen presentation, a number of highly synchronized events must first take place intracellulary. The monomorphic protein, invariant chain (Ii), is a crucial participant in MHC class II antigen presentation. Acting as a molecular chaperone, this molecule escorts the newly synthesized class II heterodimers from the endoplasmic reticulum into the endosomal system. During this manoeuvre, the interaction of li with class II serves to prevent premature association of antigenic peptide. Once the complex reaches the acidic environment of the endosomes, li is proteolytically degraded and dissociates, leaving the class II binding site available for binding antigenic peptide derived from exogenous proteins. The final Ii fragment to be displaced. CLIP (class II-associated invariant chain peptides), must be physically removed from the class II binding groove with assistance from another MHC-encoded molecule, DM. The interaction of DM with class II also aids in the subsequent rapid loading of high-affinity antigen-derived peptides into the MHC class II groove. The stable peptide-loaded complexes are now ready to exit the endocytic compartments to present their peptide antigen to specific T helper cells at the cell surface.

摘要

在过去5年里,MHC研究领域的巨大进展显著推动了我们对抗原加工途径的理解,特别是在MHC II类分子介导的抗原呈递细节方面。抗原呈递细胞表面的MHC II类分子将抗原肽呈递给CD4+辅助性T细胞。然而,为了实现有效的细胞表面抗原呈递,许多高度同步的事件必须首先在细胞内发生。单态蛋白恒定链(Ii)是MHC II类抗原呈递的关键参与者。作为一种分子伴侣,该分子将新合成的II类异二聚体从内质网护送进内体系统。在此过程中,Ii与II类分子的相互作用可防止抗原肽过早结合。一旦复合物到达内体的酸性环境,Ii就会被蛋白水解降解并解离,使II类分子的结合位点可用于结合源自外源蛋白的抗原肽。最后要被置换的Ii片段,即II类相关恒定链肽(CLIP),必须在另一种MHC编码分子DM的协助下从II类分子的结合槽中物理移除。DM与II类分子的相互作用也有助于随后将高亲和力的抗原衍生肽快速加载到MHC II类分子的凹槽中。现在,稳定的肽负载复合物准备好离开内吞区室,在细胞表面将其肽抗原呈递给特定的辅助性T细胞。

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