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由常规效应 T 细胞驱动的外周 Ly6C T 调节细胞的表型和功能变化。

Phenotypic and Functional Changes of Peripheral Ly6C T Regulatory Cells Driven by Conventional Effector T Cells.

机构信息

Academy of Immunology and Microbiology, Institute for Basic Science, Pohang, South Korea.

Department of Integrative Biosciences and Biotechnology, Pohang University of Science and Technology, Pohang, South Korea.

出版信息

Front Immunol. 2018 Mar 16;9:437. doi: 10.3389/fimmu.2018.00437. eCollection 2018.

Abstract

A relatively high affinity/avidity of T cell receptor (TCR) recognition for self-peptide bound to major histocompatibility complex II (self-pMHC) ligands is a distinctive feature of CD4 T regulatory (Treg) cells, including their development in the thymus and maintenance of their suppressive functions in the periphery. Despite such high self-reactivity, however, all thymic-derived peripheral Treg populations are neither homogenous in their phenotype nor uniformly immune-suppressive in their function under steady state condition. We show here that based on the previously defined heterogeneity in the phenotype of peripheral Treg populations, Ly6C expression on Treg marks a lower degree of activation, proliferation, and differentiation status as well as functional incompetence. We also demonstrate that Ly6C expression on Treg in a steady state is either up- or downregulated depending on relative amounts of tonic TCR signals derived from its contacts with self-ligands. Interestingly, peripheral appearance and maintenance of these Ly6C-expressing Treg cells largely differed in an age-dependent manner, with their proportion being continuously increased from perinatal to young adult period but then being gradually declined with age. The reduction of Ly6C Treg in the aged mice was not due to their augmented cell death but rather resulted from downregulation of Ly6C expression. The Ly6C downregulation was accompanied by proliferation of Ly6C Treg cells and subsequent change into Ly6C effector Treg with concomitant restoration of immune-suppressive activity. Importantly, we found that this phenotypic and functional change of Ly6C Treg is largely driven by conventional effector T cell population. Collectively, these findings suggest a potential cross-talk between peripheral Treg subsets and effector T cells and provides better understanding for Treg homeostasis and function on maintaining self-tolerance.

摘要

T 细胞受体(TCR)对与主要组织相容性复合物 II(自身-pMHC)结合的自身肽的高亲和力/亲合力是 CD4 T 调节(Treg)细胞的一个独特特征,包括它们在胸腺中的发育和在外周维持其抑制功能。然而,尽管具有如此高的自身反应性,但所有源自胸腺的外周 Treg 群体在其表型上既不是同质的,在其功能上也不是在稳态条件下普遍具有免疫抑制作用。我们在这里表明,基于先前在外周 Treg 群体表型上定义的异质性,Treg 上的 Ly6C 表达标志着较低程度的激活、增殖和分化状态以及功能无能。我们还证明,在稳态下,Treg 上的 Ly6C 表达是上调还是下调取决于其与自身配体接触所产生的紧张 TCR 信号的相对量。有趣的是,这些表达 Ly6C 的 Treg 细胞在外周的出现和维持在很大程度上以年龄依赖的方式不同,其比例从围产期到成年期持续增加,但随着年龄的增长逐渐下降。老年小鼠中 Ly6C Treg 的减少不是由于其细胞死亡的增加,而是由于 Ly6C 表达的下调。Ly6C 的下调伴随着 Ly6C Treg 细胞的增殖,随后变成 Ly6C 效应性 Treg,同时恢复免疫抑制活性。重要的是,我们发现 Ly6C Treg 的这种表型和功能变化主要是由常规效应 T 细胞群体驱动的。总的来说,这些发现表明外周 Treg 亚群和效应 T 细胞之间存在潜在的串扰,并为 Treg 稳态和维持自身耐受的功能提供了更好的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/77b7/5864862/ecd7ce3f9727/fimmu-09-00437-g001.jpg

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