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HLA-DM表达的变化影响正常B细胞系中MHC II类αβ:II类相关恒定链肽复合物向成熟的肽结合II类αβ二聚体的转化。

Variation in HLA-DM expression influences conversion of MHC class II alpha beta:class II-associated invariant chain peptide complexes to mature peptide-bound class II alpha beta dimers in a normal B cell line.

作者信息

Ramachandra L, Kovats S, Eastman S, Rudensky A Y

机构信息

Department of Immunology, University of Washington School of Medicine, Seattle 98195, USA.

出版信息

J Immunol. 1996 Mar 15;156(6):2196 - 2204.

PMID:8690909
Abstract

The maturation of invariant chain (Ii):MHC class II complexes into peptide-loaded alpha beta dimers occurs by proteolytic removal of Ii chain and binding of antigenic peptides derived from exogenous and endogenous Ags. A fragment of the Ii chain (class II-associated invariant chain peptide (CLIP) remains associated with class II alpha beta and is an intermediate in this process. Conversion of alpha beta:CLIP complexes into alpha beta:peptide complexes is facilitated by HLA-DM. Two unique mAbs, specific for I-Ab bound to human CLIP and I-Ab bound to DR alpha peptide, were used to assess the formation of these peptide:class II complexes in a human B lymphoblastoid cell line (B-LCL) (Swei) transfected with I-A(b). In multiple independent Swei:I-Ab transfectants, the amount of human CLIP (hCLIP):I-Ab expressed was inversely proportional to the amount of DR alpha 52-68:I-Ab; quantitative differences in HLA-DM expression accounted for this phenotype. In the low DM transfectant, a substantial proportion of I-Ab, but not DR molecules, was altered structurally and unable to present native protein Ags. Addition of DM transgenes to the DM-low cells resulted in an increase in DR alpha 52-68:I-Ab coupled with a decrease in hCLIP:I-Ab complexes and restoration of exogenous protein Ag presentation. The DR5 molecules in Swei cells, which have a lower affinity for hCLIP than I-Ab, were not affected by low DM expression, suggesting that the amount of DM required for conversion of CLIP:class II to peptide:class II may depend on the affinity of the class II molecules for CLIP or DM.

摘要

恒定链(Ii):MHC II类复合物成熟为负载肽的αβ二聚体是通过Ii链的蛋白水解去除以及源自外源性和内源性抗原的抗原肽的结合来实现的。Ii链的一个片段(II类相关恒定链肽(CLIP))仍与II类αβ相关联,并且是该过程中的一个中间体。HLA-DM促进αβ:CLIP复合物向αβ:肽复合物的转化。两种独特的单克隆抗体,分别针对与人CLIP结合的I-Ab和与DRα肽结合的I-Ab,用于评估在转染了I-A(b)的人B淋巴母细胞系(B-LCL)(Swei)中这些肽:II类复合物的形成。在多个独立的Swei:I-Ab转染子中,表达的人CLIP(hCLIP):I-Ab的量与DRα52-68:I-Ab的量成反比;HLA-DM表达的定量差异解释了这种表型。在低DM转染子中,相当一部分I-Ab分子,而不是DR分子,在结构上发生了改变,无法呈递天然蛋白质抗原。向低DM细胞中添加DM转基因导致DRα52-68:I-Ab增加,同时hCLIP:I-Ab复合物减少,并且恢复了外源性蛋白质抗原呈递。Swei细胞中的DR5分子对hCLIP的亲和力低于I-Ab,不受低DM表达的影响,这表明将CLIP:II类转化为肽:II类所需的DM量可能取决于II类分子对CLIP或DM的亲和力。

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