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首页> 外文期刊>Current topics in microbiology and immunology >The CD4/CD8 Lineages: Central Decisions and Peripheral Modifications for T Lymphocytes
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The CD4/CD8 Lineages: Central Decisions and Peripheral Modifications for T Lymphocytes

机译:CD4 / CD8谱系:用于T淋巴细胞的中央决策和外围修饰

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摘要

CD4~+ helper and CD8~+ cytotoxic T cells, two major subsets of alphabetaTCR expressing lymphocytes, are differentiated from common precursor CD4~+CD8~+ double-positive (DP) thymocytes. Bifurcation of the CD4~+/CD8~+ lineages in the thymus is a multilayered process and is thought to culminate in a loss of developmental plasticity between these functional subsets. Advances in the last decade have deepened our understanding of the transcription control mechanisms governing CD4 versus CD8 lineage commitment. Reciprocal expression and antagonistic interplay between two transcription factors, ThPOK and Runx3, is crucial for driving thymocyte decisions between these two cell fates. Here, we first focus on the regulation of ThPOK expression and its role in directing helper T cell development. We then discuss a novel aspect of the ThPOK/Runx3 axis in modifying CD4~+ T cell function upon exposure to gut microenvironment.
机译:CD4〜+辅助杆和CD8〜+细胞毒性T细胞,两种表达淋巴细胞的主要亚群,与常见前体CD4〜+ CD8 +双阳性(DP)胸腺细胞分化。 胸腺中CD4〜+ / CD8〜+谱系的分叉是一种多层过程,被认为在这些功能子集之间的发育可塑性丧失。 过去十年的进展深化了我们对CD4与CD8血统承诺的转录控制机制的理解。 在两个转录因子,THPOK和RUNX3之间的互易表达和拮抗相互作用对于在这两个细胞序列之间驱动胸腺细胞决策至关重要。 在这里,我们首先关注THPOK表达的调节及其在指导辅助T细胞发展中的作用。 然后,我们在暴露于肠道微环境时改变CD4〜+ T细胞功能的THPOK / RUNX3轴的新颖方面。

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