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T细胞多样性的稳态

Homeostasis of T cell diversity.

作者信息

Mahajan Vinay S, Leskov Ilya B, Chen Jian Zhu

机构信息

Center for Cancer Research and Department of Biology, Massachusetts Institute of Technology, Cambridge, 02139, USA.

出版信息

Cell Mol Immunol. 2005 Feb;2(1):1-10.

PMID:16212905
Abstract

T cell homeostasis commonly refers to the maintenance of relatively stable T cell numbers in the peripheral lymphoid organs. Among the large numbers of T cells in the periphery, T cells exhibit structural diversity, i.e., the expression of a diverse repertoire of T cell receptors (TCRs), and functional diversity, i.e., the presence of T cells at naive, effector, and memory developmental stages. Although the homeostasis of T cell numbers has been extensively studied, investigation of the mechanisms underlying the maintenance of structural and functional diversity of T cells is still at an early stage. The fundamental feature throughout T cell development is the interaction between the TCR and either self or foreign peptides in association with MHC molecules. In this review, we present evidence showing that homeostasis of T cell number and diversity is mediated through competition for limiting resources. The number of T cells is maintained through competition for limiting cytokines, whereas the diversity of T cells is maintained by competition for self-peptide-MHC complexes. In other words, diversity of the self-peptide repertoire limits the structural (TCR) diversity of a T cell population. We speculate that cognate low affinity self-peptides, acting as weak agonists and antagonists, regulate the homeostasis of T cell diversity whereas non-cognate or null peptides which are extremely abundant for any given TCR, may contribute to the homeostasis of T cell number by providing survival signals. Moreover, self-peptides and cytokines may form specialized niches for the regulation of T cell homeostasis.

摘要

T细胞稳态通常是指外周淋巴器官中T细胞数量维持相对稳定。在外周大量的T细胞中,T细胞表现出结构多样性,即多种T细胞受体(TCR)的表达,以及功能多样性,即存在处于初始、效应和记忆发育阶段的T细胞。尽管T细胞数量的稳态已得到广泛研究,但对T细胞结构和功能多样性维持机制的研究仍处于早期阶段。T细胞发育过程的基本特征是TCR与自身或外来肽与MHC分子结合的相互作用。在本综述中,我们提供证据表明,T细胞数量和多样性的稳态是通过对有限资源的竞争来介导的。T细胞数量通过对有限细胞因子的竞争得以维持,而T细胞的多样性则通过对自身肽-MHC复合物的竞争来维持。换句话说,自身肽库的多样性限制了T细胞群体的结构(TCR)多样性。我们推测,同源低亲和力自身肽作为弱激动剂和拮抗剂,调节T细胞多样性的稳态,而对于任何给定的TCR来说极其丰富的非同源或无效肽,可能通过提供存活信号来促进T细胞数量的稳态。此外,自身肽和细胞因子可能形成调节T细胞稳态的特殊微环境。

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