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在存在其MHC配体的情况下,抗原/MHC特异性T细胞优先从胸腺输出。

Antigen/MHC-specific T cells are preferentially exported from the thymus in the presence of their MHC ligand.

作者信息

Berg L J, Pullen A M, Fazekas de St Groth B, Mathis D, Benoist C, Davis M M

机构信息

Department of Microbiology and Immunology, Stanford University School of Medicine, California 94305.

出版信息

Cell. 1989 Sep 22;58(6):1035-46. doi: 10.1016/0092-8674(89)90502-3.

Abstract

Transgenic mice expressing a T cell receptor heterodimer specific for a fragment of pigeon cytochrome c plus an MHC class II molecule (I-Ek) have been made. We find that H-2k alpha beta transgenic mice have an overall increase in the number of T cells and express a 10-fold higher fraction of cytochrome c-reactive cells than H-2b mice. Surface staining of thymocytes indicates that in H-2b mice, T cell development is arrested at an intermediate stage of differentiation (CD4+8+, CD310). Analyses of mice carrying these T cell receptor genes and MHC class II I-E alpha constructs indicate that his developmental block can be reversed in H-2b mice by I-E expression on cortical epithelial cells of the thymus. These data suggest that a direct T cell receptor-MHC interaction occurs in the thymus in the absence of nominal antigen and results in the enhanced export of T cells, consistent with the concept of "positive selection".

摘要

已培育出表达对鸽细胞色素c片段特异的T细胞受体异二聚体以及MHC II类分子(I-Ek)的转基因小鼠。我们发现,H-2kαβ转基因小鼠的T细胞数量总体增加,并且与H-2b小鼠相比,表达细胞色素c反应性细胞的比例高10倍。胸腺细胞的表面染色表明,在H-2b小鼠中,T细胞发育停滞在分化的中间阶段(CD4+8+,CD310)。对携带这些T细胞受体基因和MHC II类I-Eα构建体的小鼠进行的分析表明,通过胸腺皮质上皮细胞上的I-E表达,H-2b小鼠中的这种发育阻滞可以被逆转。这些数据表明,在不存在名义抗原的情况下,胸腺中发生了直接的T细胞受体-MHC相互作用,并导致T细胞输出增强,这与“阳性选择”的概念一致。

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