上皮干细胞谱系的Treg调控

Inchul Cho , Prudence Pokwai Lui , Niwa Ali
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引用次数: 10

摘要

成体生物的组织修复和维持依赖于干细胞(SCs)与其微环境或生态位组成细胞之间的相互作用。越来越多的证据表明,免疫细胞,特别是Foxp3+ CD4+调节性T细胞(Tregs),在SC生态位的调节中起着重要作用。毋庸置疑,treg是CD4+ T细胞室的主要免疫抑制谱系,存在于许多次级淋巴器官中,在那里它们发挥作用。这些细胞还专门用于促进其居住组织特有的保护功能。在这篇综述中,我们讨论了在稳态和sc介导的再生过程中支持组织驻留treg的sc调节功能的新兴概念。我们强调皮肤、肠和肺是受反复微损伤、暴露于微生物群并不断被常驻干细胞群补充的模型器官。深入了解Treg-SC轴的生物学将为正在进行的针对组织驻留treg的特定亚群的免疫治疗工作提供信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Treg regulation of the epithelial stem cell lineage

Tissue repair and maintenance in adult organisms is dependent on the interactions between stem cells (SCs) and constituent cells of their microenvironment, or niche. Accumulating evidence suggests that immune cells, specifically Foxp3+ CD4+ Regulatory T cells (Tregs), play an important role as a regulator of the SC niche. Undisputedly, Tregs are the major immunosuppressive lineage of the CD4+ T cell compartment, and reside within numerous secondary lymphoid organs, where they exert their functions. These cells are also specialised in facilitating protective functions specific to their tissue of residence. In this review, we discuss the emerging concepts supporting the SC-regulatory functions of tissue-resident Tregs, during both the steady-state and SC-mediated regeneration. We highlight the skin, intestines, and lung as model organs which are subject to recurrent microinjury,exposure to microbiota, and constantly replenished by resident stem cell populations. An in-depth understanding of the biology of the Treg-SC axis will inform ongoing immunotherapeutic endeavours to target specific subpopulations of tissue-resident Tregs.

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