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T淋巴细胞成熟亚群分化中随机机制的证据。

Evidence for a stochastic mechanism in the differentiation of mature subsets of T lymphocytes.

作者信息

Davis C B, Killeen N, Crooks M E, Raulet D, Littman D R

机构信息

Department of Microbiology and Immunology, University of California, San Francisco 94143-0414.

出版信息

Cell. 1993 Apr 23;73(2):237-47. doi: 10.1016/0092-8674(93)90226-g.

Abstract

Thymocytes that coexpress the CD4 and CD8 glycoproteins differentiate into mature CD4+ helper or CD8+ cytotoxic cells depending on whether their antigen receptors are specific for MHC class II or class I molecules, respectively. The mechanism of this decision process was investigated in mice whose T cell development was biased toward the class II-specific lineage. We found that constitutive expression of CD4 allows a developmentally arrested population of thymocytes that have mismatched class II-specific TCRs and the CD8 coreceptor to be rescued and to acquire a cytotoxic phenotype. This result is consistent with a two-step process of thymocyte maturation, in which there is stochastic down-regulation of either CD4 or CD8 and subsequent selection based on the ability of the TCR and remaining coreceptor to engage the same MHC molecule.

摘要

共表达CD4和CD8糖蛋白的胸腺细胞会分化为成熟的CD4+辅助性细胞或CD8+细胞毒性细胞,这分别取决于它们的抗原受体是否对MHC II类或I类分子具有特异性。在T细胞发育偏向II类特异性谱系的小鼠中研究了这一决定过程的机制。我们发现,CD4的组成性表达可使一群发育停滞的胸腺细胞得到拯救,这些胸腺细胞具有不匹配的II类特异性TCR和CD8共受体,并获得细胞毒性表型。这一结果与胸腺细胞成熟的两步过程一致,即在该过程中,CD4或CD8会随机下调,随后根据TCR和剩余共受体与同一MHC分子结合的能力进行选择。

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