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TCR Vγ9链库的进化与功能:公开有益。

Evolution and function of the TCR Vgamma9 chain repertoire: It's good to be public.

作者信息

Pauza C David, Cairo Cristiana

机构信息

Institute of Human Virology, University of Maryland School of Medicine, Baltimore, MD 21201, USA.

Institute of Human Virology, University of Maryland School of Medicine, Baltimore, MD 21201, USA.

出版信息

Cell Immunol. 2015 Jul;296(1):22-30. doi: 10.1016/j.cellimm.2015.02.010. Epub 2015 Mar 4.

Abstract

Lymphocytes expressing a T cell receptor (TCR) composed of Vgamma9 and Vdelta2 chains represent a minor fraction of human thymocytes. Extrathymic selection throughout post-natal life causes the proportion of cells with a Vgamma9-JP rearrangement to increase and elevates the capacity for responding to non-peptidic phosphoantigens. Extrathymic selection is so powerful that phosphoantigen-reactive cells comprise about 1 in 40 circulating memory T cells in healthy adults and the subset expands rapidly upon infection or in response to malignancy. Skewing of the gamma delta TCR repertoire is accompanied by selection for public gamma chain sequences such that many unrelated individuals overlap extensive in their circulating repertoire. This type of selection implies the presence of a monomorphic antigen-presenting molecule that is an object of current research but remains incompletely defined. While selection on a monomorphic presenting molecule may seem unusual, similar mechanisms shape the alpha beta T cell repertoire including the extreme examples of NKT or mucosal-associated invariant T cells (MAIT) and the less dramatic amplification of public Vbeta chain rearrangements driven by individual MHC molecules and associated with resistance to viral pathogens. Selecting and amplifying public T cell receptors whether alpha beta or gamma delta, are important steps in developing an anticipatory TCR repertoire. Cell clones expressing public TCR can accelerate the kinetics of response to pathogens and impact host survival.

摘要

表达由Vγ9和Vδ2链组成的T细胞受体(TCR)的淋巴细胞仅占人类胸腺细胞的一小部分。出生后的胸腺外选择会导致具有Vγ9-JP重排的细胞比例增加,并提高对非肽磷抗原的反应能力。胸腺外选择的作用非常强大,以至于在健康成年人中,磷抗原反应性细胞约占循环记忆T细胞的四十分之一,并且该亚群在感染或对恶性肿瘤作出反应时会迅速扩增。γδTCR库的偏向伴随着对共有γ链序列的选择,因此许多不相关的个体在其循环库中有广泛的重叠。这种选择意味着存在一种单态抗原呈递分子,这是当前研究的对象,但仍未完全明确。虽然在单态呈递分子上进行选择似乎不寻常,但类似的机制塑造了αβT细胞库,包括NKT或黏膜相关恒定T细胞(MAIT)等极端例子,以及由个体MHC分子驱动并与抗病毒病原体抗性相关的共有Vβ链重排的不太显著的扩增。选择和扩增共有T细胞受体,无论是αβ还是γδ,都是发展预期TCR库的重要步骤。表达共有TCR的细胞克隆可以加快对病原体的反应动力学并影响宿主存活。

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