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一种用于MHC II类肽受体恒定链介导组装的修订模型。

A revised model for invariant chain-mediated assembly of MHC class II peptide receptors.

作者信息

Koch Norbert, McLellan Alexander D, Neumann Jürgen

机构信息

Division of Immunobiology, Institute of Genetics, University of Bonn, Bonn, Germany.

出版信息

Trends Biochem Sci. 2007 Dec;32(12):532-7. doi: 10.1016/j.tibs.2007.09.007. Epub 2007 Nov 5.

Abstract

The enormous number of allelic MHC class II glycoproteins provides the immune system with a large set of heterodimeric receptors for the binding of pathogen-derived peptides. How do inherited allo- or isotypic subunits of MHC class II combine to produce such a variety of functional peptide receptors? We propose a new mechanism in which pairing of matched MHC class II alpha- and beta-subunits is coordinated by the invariant chain chaperone. The assembly is proposed to occur in a sequential fashion, with a matched beta-chain being selected by the alpha-chain-invariant chain 'scaffold' complex that is formed first. This sequential assembly is a prerequisite for subsequent intracellular transport of the alpha-chain-invariant chain-beta-oligomer and its maturation into a functional peptide receptor.

摘要

大量的等位基因MHC II类糖蛋白为免疫系统提供了一大组用于结合病原体衍生肽的异二聚体受体。MHC II类的遗传同种异体或同型亚基是如何结合以产生如此多样的功能性肽受体的呢?我们提出了一种新机制,即匹配的MHC II类α和β亚基的配对由恒定链伴侣协调。组装过程被认为是以一种顺序方式发生的,首先形成的α链-恒定链“支架”复合物会选择匹配的β链。这种顺序组装是随后α链-恒定链-β寡聚体进行细胞内运输并成熟为功能性肽受体的先决条件。

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