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首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Mouse and human CD8(+) CD28(low) regulatory T lymphocytes differentiate in the thymus
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Mouse and human CD8(+) CD28(low) regulatory T lymphocytes differentiate in the thymus

机译:小鼠和人CD8(+)CD28(低)调节性T淋巴细胞在胸腺中分化

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摘要

Regulatory T (Treg) lymphocytes play a central role in the control of immune responses and so maintain immune tolerance and homeostasis. In mice, expression of the CD8 co-receptor and low levels of the co-stimulatory molecule CD28 characterizes a Treg cell population that exerts potent suppressive function in vitro and efficiently controls experimental immunopathology in vivo. It has remained unclear if CD8(+) CD28(low) Treg cells develop in the thymus or represent a population of chronically activated conventional T cells differentiating into Treg cells in the periphery, as suggested by their CD28(low) phenotype. We demonstrate that functional CD8(+) CD28(low) Treg cells are present in the thymus and that these cells develop locally and are not recirculating from the periphery. Differentiation of CD8(+) CD28(low) Treg cells requires MHC class I expression on radioresistant but not on haematopoietic thymic stromal cells. In contrast to other Treg cells, CD8(+) CD28(low) Treg cells develop simultaneously with CD8(+) CD28(hig)h conventional T cells. We also identified a novel homologous naive CD8(+) CD28(low) T-cell population with immunosuppressive properties in human blood and thymus. Combined, our data demonstrate that CD8(+) CD28(low) cells can develop in the thymus of mice and suggest that the same is true in humans.
机译:调节性T(Treg)淋巴细胞在控制免疫反应中起着核心作用,因此可以维持免疫耐受性和体内平衡。在小鼠中,CD8共受体的表达和低水平的共刺激分子CD28表征了Treg细胞群,该细胞群在体外发挥着强大的抑制功能,并有效地控制了体内的实验免疫病理学。尚不清楚CD8(+)CD28(低)Treg细胞是否在胸腺中发育,或代表一群长期激活的常规T细胞分化为外周Treg细胞,正如其CD28(低)表型所暗示的那样。我们证明,在胸腺中存在功能性CD8(+)CD28(低)Treg细胞,并且这些细胞在局部发育,不会从周围循环。 CD8(+)CD28(低)Treg细胞的分化需要在放射抗性而非造血胸腺基质细胞上表达MHC I类。与其他Treg细胞相反,CD8(+)CD28(低)Treg细胞与CD8(+)CD28(hig)h传统T细胞同时发育。我们还确定了在人类血液和胸腺中具有免疫抑制特性的新型同源天然CD8(+)CD28(low)T细胞群体。综合起来,我们的数据表明CD8(+)CD28(low)细胞可以在小鼠的胸腺中发育,并暗示在人类中也是如此。

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