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The majority of postselection CD4+ single-positive thymocytes requires the thymus to produce long-lived functional T cells

机译:大多数选择后CD4 +单阳性胸腺细胞都需要胸腺产生长寿的功能性T细胞

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摘要

We have previously isolated, and characterized in vitro, two subsets of CD4hi T cell receptor (TCR)hi single positive (SP) thymocytes: CD8- and CD8lo. In this report, we have analyzed phenotypic, functional, and developmental characteristics of these "late" CD4hi SP thymocyte subsets. The TCRhi phenotype and the elimination of T cells expressing TCR V beta segments reactive with endogenous mouse mammary tumor virus (MMTV) products suggested that both subsets had undergone positive and negative selection. CD8-4hi thymocytes were functional, as judged by their ability to: (a) induce lethal graft versus host disease (GVHD); (b) survive and expand in peripheral lymphoid organs; and (c) proliferate, rather than undergo apoptosis, in response to in vitro TCR cross-linking. By contrast, CD8lo4hi cells could not induce GVHD, were unable to expand (and perhaps even survive) in peripheral organs and underwent apoptosis upon TCR cross-linking. However, when reintroduced into the thymus, these cells matured into functional, long-lived CD8- 4hi lymphocytes. These results document an obligatory requirement for the thymic microenvironment in the final maturation of the majority of CD4hi SP postselection thymocytes, and demonstrate the existence of a previously unrecognized control point in T cell development.
机译:我们以前已经分离并在体外鉴定了CD4hi T细胞受体(TCR)hi单阳性(SP)胸腺细胞的两个子集:CD8-和CD8lo。在本报告中,我们分析了这些“晚期” CD4hi SP胸腺细胞亚群的表型,功能和发育特征。 TCRhi表型和表达TCR Vβ片段与内源性小鼠乳腺肿瘤病毒(MMTV)产品反应的T细胞的消除表明这两个子集都经历了正选择和负选择。根据CD8-4hi胸腺细胞的功能,它们具有以下功能:(a)诱导致死性移植物抗宿主病(GVHD); (b)在周围的淋巴器官中存活并扩大; (c)响应体外TCR交联而增殖,而不是发生凋亡。相比之下,CD8lo4hi细胞不能诱导GVHD,不能在外周器官中扩增(甚至存活),并且在TCR交联时发生凋亡。然而,当重新引入胸腺时,这些细胞成熟为功能性,长寿命的CD8-4hi淋巴细胞。这些结果证明了大多数CD4hi SP筛选后胸腺细胞在最终成熟中对胸腺微环境的强制性要求,并证明了T细胞发育中存在先前无法识别的控制点。

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