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肠道上皮内淋巴细胞的两个亚群中T细胞受体转导模块的不同使用与T细胞分化的不同途径相关。

Different use of T cell receptor transducing modules in two populations of gut intraepithelial lymphocytes are related to distinct pathways of T cell differentiation.

作者信息

Guy-Grand D, Rocha B, Mintz P, Malassis-Seris M, Selz F, Malissen B, Vassalli P

机构信息

Institut National de la Santé et de la Recherche Médicale (INSERM) U.132, Hôpital Necker-Enfants Malades, Paris, France.

出版信息

J Exp Med. 1994 Aug 1;180(2):673-9. doi: 10.1084/jem.180.2.673.

Abstract

Most gut intraepithelial cells (IEL) of the mouse are T cells that bear CD8 molecules, present either as alpha-beta chain heterodimers (CD8 beta+) or as alpha chain homodimers (CD8 beta-). All CD8 beta+ IEL bear alpha/beta T cell receptors (TCR); CD8 beta- IEL bear either alpha/beta or gamma/delta TCR and are considered to be a thymus-independent (TI) population, probably arising locally from a small fraction of CD3- IEL containing the recombinant activating gene RAG proteins. Here we report that TI CD8 beta- IEL, whether bearing alpha/beta or gamma/delta TCR, contain, in normal mice, mRNAs for both zeta and Fc epsilon RI gamma chains. These chains are present in their CD3-TCR complexes as homo- or heterodimers. In contrast, only zeta chain mRNA and homodimers are found in gut CD8 alpha/beta+ IEL and in peripheral T lymphocytes. Intestinal CD3- precursor cells contain only gamma chain, and CD3- IL-2R+ thymocyte precursors only zeta chain mRNAs. Only very primitive thymocyte precursors contain detectable gamma chain mRNA, and it thus appears that Fc epsilon RI gamma chain use is switched off at a very early stage during thymocyte differentiation. Thus, T cell differentiation in the gut epithelium differs from that occurring in the thymus, from which CD8 beta+ IEL appear to derive. Use of different TCR transducing modules and CD8 accessory molecules between the TI and the thymus-derived T cell populations provides an explanation for their difference in reactivity to antigenic stimulations and thus in selection of repertoires.

摘要

小鼠的大多数肠道上皮内淋巴细胞(IEL)是带有CD8分子的T细胞,这些CD8分子以α-β链异二聚体(CD8β+)或α链同二聚体(CD8β-)的形式存在。所有CD8β+ IEL都带有α/β T细胞受体(TCR);CD8β- IEL带有α/β或γ/δ TCR,被认为是不依赖胸腺的(TI)群体,可能局部起源于一小部分含有重组激活基因RAG蛋白的CD3- IEL。在此我们报告,在正常小鼠中,无论带有α/β还是γ/δ TCR,TI CD8β- IEL都含有ζ链和FcεRIγ链的mRNA。这些链以同二聚体或异二聚体的形式存在于它们的CD3-TCR复合物中。相比之下,在肠道CD8α/β+ IEL和外周T淋巴细胞中仅发现ζ链mRNA和同二聚体。肠道CD3-前体细胞仅含有γ链mRNA,而CD3- IL-2R+胸腺细胞前体细胞仅含有ζ链mRNA。只有非常原始的胸腺细胞前体含有可检测到的γ链mRNA,因此似乎FcεRIγ链的使用在胸腺细胞分化的非常早期阶段就被关闭了。因此,肠道上皮中的T细胞分化不同于胸腺中的T细胞分化,CD8β+ IEL似乎来源于胸腺。TI和胸腺来源的T细胞群体之间不同TCR转导模块和CD8辅助分子的使用,为它们对抗原刺激的反应性差异以及因此在 repertoire 选择上的差异提供了解释。

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