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缺乏恒定链表达的小鼠中主要组织相容性复合体II类组装、运输、肽获取及CD4+ T细胞选择存在缺陷。

Defective major histocompatibility complex class II assembly, transport, peptide acquisition, and CD4+ T cell selection in mice lacking invariant chain expression.

作者信息

Bikoff E K, Huang L Y, Episkopou V, van Meerwijk J, Germain R N, Robertson E J

机构信息

Department of Cellular and Developmental Biology, Harvard University, Cambridge, Massachusetts 02138.

出版信息

J Exp Med. 1993 Jun 1;177(6):1699-712. doi: 10.1084/jem.177.6.1699.

Abstract

We used gene targeting techniques to produce mice lacking the invariant chain associated with major histocompatibility complex (MHC) class II molecules. Cells from these mice show a dramatic reduction in surface class II, resulting from both defective association of class II alpha and beta chains and markedly decreased post-Golgi transport. The few class II alpha/beta heterodimers reaching the cell surface behave as if empty or occupied by an easily displaced peptide, and display a distinct structure. Mutant spleen cells are defective in their ability to present intact protein antigens, but stimulate enhanced responses in the presence of peptides. These mutant mice have greatly reduced numbers of thymic and peripheral CD4+ T cells. Overall, this striking phenotype establishes that the invariant chain plays a critical role in regulating MHC class II expression and function in the intact animal.

摘要

我们运用基因靶向技术培育出了缺乏与主要组织相容性复合体(MHC)II类分子相关的恒定链的小鼠。这些小鼠的细胞表面II类分子显著减少,这是由于II类α链和β链的结合存在缺陷以及高尔基体后转运明显减少所致。少数到达细胞表面的II类α/β异二聚体表现得似乎是空的或被一个易于置换的肽所占据,并呈现出独特的结构。突变的脾细胞在呈递完整蛋白质抗原的能力上存在缺陷,但在有肽存在的情况下能刺激增强的反应。这些突变小鼠胸腺和外周CD4 + T细胞的数量大幅减少。总体而言,这种显著的表型表明恒定链在完整动物中调节MHC II类分子的表达和功能方面起着关键作用。

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