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在外源蛋白抗原呈递缺陷的细胞中,自身肽与MHC II类分子之间复合物的形成。

Formation of complexes between self-peptides and MHC class II molecules in cells defective for presentation of exogenous protein antigens.

作者信息

Bikoff E K

机构信息

Department of Obstetrics, Gynecology, and Reproductive Sciences, Mount Sinai School of Medicine, New York, NY 10029.

出版信息

J Immunol. 1992 Jul 1;149(1):1-8.

PMID:1318896
Abstract

A vertebrate immune response is initiated by the presentation of foreign protein Ag to MHC class II-restricted T lymphocytes by specialized APC. Presentation of self-peptides in association with MHC class II molecules is also necessary for the induction of T cell tolerance. It is important to understand whether functionally divergent APC are responsible for delivering these distinct signals to class II-restricted T cells. Here we examine the ability of I-Ad surface molecules expressed in diverse cell types to stimulate I-Ad-restricted T cells. Recipients included J558L myeloma cells and EL4 lymphoma cells expressing barely detectable or undetectable levels of Ii chain mRNA. This allowed us to examine the influence of Ii expression on the presentation of intracellular Ag and thus test the hypothesis that Ii chain is necessary to prevent access of self-peptides to newly synthesized class II molecules. Ii chain expression did not restore the ability of transformants to process and present soluble protein Ag. A striking result was the finding that cells showing a defect in the exogenous class II presentation pathway were capable of functioning as stimulators when they expressed intracellular secreted but not signal-less V-CH3b Ag. Thus, so-called professional APC that can capture and process exogenous protein Ag may express a specialized set of proteins not required for the presentation of self-peptides.

摘要

脊椎动物的免疫反应是由特殊的抗原呈递细胞(APC)将外来蛋白质抗原呈递给MHC II类限制性T淋巴细胞而启动的。与MHC II类分子结合呈递自身肽对于诱导T细胞耐受性也是必需的。了解功能不同的APC是否负责将这些不同的信号传递给II类限制性T细胞非常重要。在这里,我们研究了在不同细胞类型中表达的I-Ad表面分子刺激I-Ad限制性T细胞的能力。受体包括J558L骨髓瘤细胞和EL4淋巴瘤细胞,它们表达的Ii链mRNA水平几乎检测不到或无法检测到。这使我们能够研究Ii表达对细胞内抗原呈递的影响,从而检验Ii链对于防止自身肽接近新合成的II类分子是必需的这一假设。Ii链表达并未恢复转化体加工和呈递可溶性蛋白质抗原的能力。一个惊人的结果是发现,在外源性II类呈递途径中存在缺陷的细胞,当它们表达细胞内分泌但无信号的V-CH3b抗原时,能够作为刺激细胞发挥作用。因此,能够捕获和加工外源性蛋白质抗原的所谓专职APC可能表达一组呈递自身肽所不需要的特殊蛋白质。

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