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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Thymic Origins of T Cell Receptor Alloreactivity
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Thymic Origins of T Cell Receptor Alloreactivity

机译:T细胞受体含有胸腺的脑渊源

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Major histocompatibility complex (MHC) restriction is a unique feature of T cell antigen recognition. Mature T cells respond to antigenic nonself peptides bound to self-MHC molecules, but a sizeable fraction of peripheral T cells can also respond to nonself peptide-MHC (pMHC) complexes in the context of transplantation. MHC specificity of the T cell receptor (TCR) repertoire is shaped during thymic development. Two hypotheses have been proposed to explain MHC specificity of T cells. It has been suggested that MHC specificity is an intrinsic feature of TCR structure, mediated by the germline-encoded regions of the TCR sequence. In support of this model, an estimated 15% to 30% of preselection TCR repertoire is estimated to be MHC-specific. Moreover, structural studies have shown some degree of conserved binding topology for TCR-peptide MHC complexes. However, there is also evidence that MHC restriction can be imposed on the TCR repertoire during thymic development, and it has been proposed that the interaction of the Lck kinase with CD4 or CD8 coreceptors is critical for generation of MHC specificity. This review will discuss recent work on assessment of the preselection of TCR repertoire, molecular evidence for the germline encoded TCR bias for MHC, and for the coreceptor sequestration model in the context of alloreactivity and transplantation.
机译:主要的组织相容性复合物(MHC)限制是T细胞抗原识别的独特特征。成熟的T细胞响应与自我MHC分子结合的抗原不良肽,但在移植的背景下,大量的外周T细胞也可以响应Nonself肽-MHC(PMHC)复合物。 T细胞受体(TCR)曲目的MHC特异性在胸腺发育过程中成形。已经提出了两个假设来解释T细胞的MHC特异性。已经提出,MHC特异性是TCR结构的内在特征,由TCR序列的种系编码区域介导。为了支持该模型,估计的15%至30%的预选TCR曲目估计是MHC特异性的。此外,结构研究表明了TCR-肽MHC复合物的一定程度的保守结合拓扑。然而,还有证据表明,MHC限制可以在胸腺发育期间对TCR曲目施加,并且已经提出了LCK激酶与CD4或CD8团簇的相互作用对于产生MHC特异性至关重要。本综述将讨论最近关于评估TCR曲目的预选的工作,用于MHC的种系编码的TCR偏差的分子证据,以及在均法和移植的背景下的团簇螯合模型。

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