胸腺上皮诱导耐受的机制研究。

V Thomas-Vaslin, M Coltey, J Salaün
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摘要

我们设计了一种模型,在裸鼠出生时,通过皮下移植从10天的异体胚胎中取出的胚胎胸腺上皮(TE)来重建T细胞。TE由分化为T细胞的裸鼠造血细胞定植。这种T细胞重组的裸鼠能够排斥第三方皮肤移植,并且对自身单倍型皮肤和TE H-2型皮肤具有耐受性。我们最近的研究表明,这种耐受性可以通过选择在同种异体TE上的CD4+外周T细胞转移。关于这些T细胞是否可以调节来自正常小鼠的效应细胞的活性的问题在这里得到了解决。我们发现,将来自这种嵌合体的外周T细胞与来自正常小鼠的同基因T细胞一起转移到裸受体中,可显著延缓TE单倍型皮肤移植的排斥反应。这种延迟取决于两种注射细胞的比例。这表明,在同种异体TE上选择的调节性T细胞能够控制正常小鼠外周血T细胞的效应活性。因此,在同种异体TE上选择的T细胞可以被认为在导致效应细胞激活的过程中具有负调控活性。
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On the mechanisms of thymic epithelium induced tolerance.

We have devised a model in which nude mice are T cell reconstituted at birth by subcutaneous grafts of embryonic thymic epithelium (TE) removed from 10 days allogeneic embryos. The TE is colonized by the nude mouse hemopoietic cells which differentiate into T cells. Such T cell-reconstituted nude mice are able to reject third party skin graft and are tolerant to skin of their own haplotype but also the TE H-2 type. We have recently shown that this tolerance can be transferred by CD4+ peripheral T cells selected on the allogeneic TE. The question as to whether such T cells can regulate the activity of effector cells from normal mice is addressed here. We show that the transfer of peripheral T cells issued from such chimeras, together with syngeneic T cells from normal mice, into nude recipients induces a significant delay in the rejection of skin graft of the TE haplotype. This delay depends on the ratio of the 2 types of injected cells. This demonstrates that regulatory T cells selected on an allogeneic TE are able to control the effector activity of peripheral T cells issued from normal mice. The T cells selected on the allogeneic TE can therefore be considered as endowed with a negative regulatory activity with respect to the process leading to effector cells activation.

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