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发育过程中TCRVα链的受体特异性等位基因排斥

Receptor-specific allelic exclusion of TCRV alpha-chains during development.

作者信息

Boyd R, Kozieradzki I, Chidgey A, Mittrücker H W, Bouchard D, Timms E, Kishihara K, Ong C J, Chui D, Marth J D, Mak T W, Penninger J M

机构信息

Department of Pathology and Immunology, Monash Medical School, Melbourne, Victoria, Australia.

出版信息

J Immunol. 1998 Aug 15;161(4):1718-27.

PMID:9712036
Abstract

Expression of a single Ag receptor on lymphocytes is maintained via allelic exclusion that generates cells with a clonal receptor repertoire. We show in normal mice and mice expressing functionally rearranged TCR alphabeta transgenes that allelic exclusion at the TCR alpha locus is not operational in immature thymocytes, whereas most mature T cells express a single TCRV alpha-chain. TCRV alpha allelic exclusion in mature thymocytes is regulated through a CD45 tyrosine phosphatase-mediated signal during positive selection. Using functional and genetic systems for selection of immature double TCRV alpha+ thymocytes, we show that peptide-specific ligand recognition provides the signal for allelic exclusion, i.e., mature T cells maintain expression of the ligand-specific TCRV alpha-chain, but lose the nonfunctional receptor. Whereas activation of TCRV beta-chains or CD3epsilon leads to receptor internalization, TCRV alpha ligation promotes retention of the TCR on the cell surface. Although both TCRV alpha- and TCRV beta-chains trigger phosphotyrosine signaling, only the TCRV beta-chain mediates membrane recruitment of the GTPase dynamin. These data indicate that TCRV alpha-directed signals for positive selection control allelic exclusion in T cells, and that developmental signals can select for single receptor usage.

摘要

淋巴细胞上单个抗原受体的表达通过等位基因排斥得以维持,这种排斥产生具有克隆受体库的细胞。我们在正常小鼠和表达功能重排的TCRαβ转基因的小鼠中发现,TCRα基因座的等位基因排斥在未成熟胸腺细胞中不起作用,而大多数成熟T细胞表达单一的TCRVα链。成熟胸腺细胞中的TCRVα等位基因排斥在阳性选择过程中通过CD45酪氨酸磷酸酶介导的信号进行调节。利用用于选择未成熟双TCRVα+胸腺细胞的功能和遗传系统,我们表明肽特异性配体识别为等位基因排斥提供信号,即成熟T细胞维持配体特异性TCRVα链的表达,但失去无功能的受体。虽然TCRVβ链或CD3ε的激活导致受体内化,但TCRVα连接促进TCR保留在细胞表面。尽管TCRVα链和TCRVβ链都触发磷酸酪氨酸信号传导,但只有TCRVβ链介导GTP酶发动蛋白的膜募集。这些数据表明,TCRVα导向的阳性选择信号控制T细胞中的等位基因排斥,并且发育信号可以选择单一受体的使用。

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