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Regulatory T-cell trafficking: from thymic development to tumor-induced immune suppression.

机译:调节性T细胞运输:从胸腺发育到肿瘤诱导的免疫抑制。

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Regulatory T cells (Tregs) have become a priority for many investigators in immunology due to their potent immunosuppressive and tolerogenic effects. While Treg activity is required for normal immune homeostasis, dysregulation of their numbers can induce autoimmunity or aid in the pathogenesis of disease. Therefore, great effort has been made to understand the mechanisms by which Tregs accumulate in different areas of the body. Like other lymphocytes, Tregs migrate in response to a network of chemotactic stimuli involving chemokines, chemokine receptors, integrins, and their corresponding ligands. However, many of these stimuli are exclusive to Tregs, inducing their migration while leaving conventional populations unaffected. It is these selective stimuli that result in increased ratios of Tregs among conventional effector populations, leading to changes in immune suppression and homeostasis. This review explores selective Treg trafficking during thymic Treg development, migration to secondary lymphoid tissues and emigration into the periphery during homeostatic conditions, inflammation, and the tumor microenvironment, placing emphasis on stimuli that selectively recruits Tregs to target locations.
机译:调节性T细胞(Tregs)由于其有效的免疫抑制和致耐受作用,已成为许多免疫学研究者的优先考虑的问题。正常的免疫稳态需要Treg活性,但其数量失调可以诱导自身免疫或帮助疾病的发病。因此,已作出巨大的努力来了解Treg在人体不同部位积聚的机制。像其他淋巴细胞一样,Treg响应于趋化因子,趋化因子受体,整联蛋白及其相应配体的趋化刺激网络而迁移。但是,这些刺激中有许多是Treg所独有的,在不影响常规人群的情况下诱导其迁移。这些选择性刺激导致常规效应子群体中Tregs的比率增加,导致免疫抑制和体内平衡的改变。这篇综述探讨了在胸腺Treg发育过程中的选择性Treg转运,在稳态条件,炎症和肿瘤微环境中迁移至次级淋巴组织以及向周边迁移的情况,重点是选择性地募集Treg到目标位置的刺激。

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