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胸腺皮质阳性选择对自身反应性调节性T细胞库的塑造

Shaping of the autoreactive regulatory T cell repertoire by thymic cortical positive selection.

作者信息

Ribot Julie, Enault Geneviève, Pilipenko Sylvie, Huchenq Anne, Calise Maryline, Hudrisier Denis, Romagnoli Paola, van Meerwijk Joost P M

机构信息

Institut National de la Santé et de la Recherche Médicale Unité 563, Toulouse, France.

出版信息

J Immunol. 2007 Nov 15;179(10):6741-8. doi: 10.4049/jimmunol.179.10.6741.

Abstract

The main function of regulatory T lymphocytes is to keep autoimmune responses at bay. Accordingly, it has been firmly established that the repertoire of CD4(+)CD25(+)Foxp3(+) regulatory T cells (Tregs) is enriched in autospecific cells. Differences in thymic-positive and/or -negative selection may account for selection of the qualitatively distinct regulatory and conventional T cell (Tconv) repertoires. It has previously been shown that precursors for Tregs are less sensitive to negative selection than Tconv precursors. Studies with TCR/ligand doubly transgenic mice suggested that an agonist ligand might induce positive selection of Treg (but not Tconv) cells. However, massive deletion of Tconv (but not Treg) cell precursors observed in these mice renders interpretation of such data problematic and a potential role for positive selection in generation of the autospecific Treg repertoire has remained therefore incompletely understood. To study this important unresolved issue and circumvent use of TCR/ligand-transgenic mice, we have developed transgenic mice expressing a single MHC class II/peptide ligand on positively selecting thymic cortical epithelial cells. We found that functional Treg (but not Tconv) cells specific for the single ligand were preferentially selected from the naturally diverse repertoire of immature precursors. Our data therefore demonstrate that thymic cortical positive selection of regulatory and Tconv precursors is governed by distinct rules and that it plays an important role in shaping the autoreactive Treg repertoire.

摘要

调节性T淋巴细胞的主要功能是抑制自身免疫反应。因此,已经明确证实,CD4(+)CD25(+)Foxp3(+)调节性T细胞(Tregs)库中富含自身特异性细胞。胸腺阳性和/或阴性选择的差异可能解释了定性不同的调节性T细胞和常规T细胞(Tconv)库的选择。此前已经表明,Tregs的前体对阴性选择的敏感性低于Tconv前体。对TCR/配体双转基因小鼠的研究表明,激动剂配体可能诱导Treg(而非Tconv)细胞的阳性选择。然而,在这些小鼠中观察到的Tconv(而非Treg)细胞前体的大量缺失使得对此类数据的解释存在问题,因此,阳性选择在自身特异性Treg库产生中的潜在作用仍未完全理解。为了研究这个重要的未解决问题并避免使用TCR/配体转基因小鼠,我们开发了在阳性选择的胸腺皮质上皮细胞上表达单一MHC II类/肽配体的转基因小鼠。我们发现,针对单一配体的功能性Treg(而非Tconv)细胞优先从未成熟前体的自然多样库中被选择。因此,我们的数据表明,调节性T细胞和Tconv前体的胸腺皮质阳性选择受不同规则支配,并且在塑造自身反应性Treg库中起重要作用。

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