Trigueros C, Ramiro A R, Carrasco Y R, de Yebenes V G, Albar J P, Toribio M L
Centro de Biología Molecular "Severo Ochoa,".
J Exp Med. 1998 Oct 19;188(8):1401-12. doi: 10.1084/jem.188.8.1401.
During thymocyte development, progression from T cell receptor (TCR)beta to TCRalpha rearrangement is mediated by a CD3-associated pre-TCR composed of the TCRbeta chain paired with pre-TCRalpha (pTalpha). A major issue is how surface expression of the pre-TCR is regulated during normal thymocyte development to control transition through this checkpoint. Here, we show that developmental expression of pTalpha is time- and stage-specific, and is confined in vivo to a limited subset of large cycling human pre-T cells that coexpress low density CD3. This restricted expression pattern allowed the identification of a novel subset of small CD3(-) thymocytes lacking surface pTalpha, but expressing cytoplasmic TCRbeta, that represent late noncycling pre-T cells in which recombination activating gene reexpression and downregulation of T early alpha transcription are coincident events associated with cell cycle arrest, and immediately preceding TCRalpha gene expression. Importantly, thymocytes at this late pre-T cell stage are shown to be functional intermediates between large pTalpha+ pre-T cells and TCRalpha/beta+ thymocytes. The results support a developmental model in which pre-TCR-expressing pre-T cells are brought into cycle, rapidly downregulate surface pre-TCR, and finally become small resting pre-T cells, before the onset of TCRalpha gene expression.
在胸腺细胞发育过程中,从T细胞受体(TCR)β重排到TCRα重排的进程是由一种与CD3相关的前TCR介导的,该前TCR由与前TCRα(pTα)配对的TCRβ链组成。一个主要问题是在正常胸腺细胞发育过程中,前TCR的表面表达是如何被调控的,以控制通过这个检查点的转变。在这里,我们表明pTα的发育表达具有时间和阶段特异性,并且在体内局限于一小部分共表达低密度CD3的大型循环人前T细胞。这种受限的表达模式使得能够鉴定出一个新的小CD3(-)胸腺细胞亚群,这些细胞缺乏表面pTα,但表达细胞质TCRβ,它们代表晚期非循环前T细胞,其中重组激活基因的重新表达和T早期α转录的下调是与细胞周期停滞相关的同时发生的事件,并且紧接在TCRα基因表达之前。重要的是,处于这个晚期前T细胞阶段的胸腺细胞被证明是大型pTα+前T细胞和TCRα/β+胸腺细胞之间的功能中间体。这些结果支持了一种发育模型,即在TCRα基因表达开始之前,表达前TCR的前T细胞进入细胞周期,迅速下调表面前TCR,最终成为小型静止前T细胞。
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