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Mechanisms of regulatory T-cell suppression – a diverse arsenal for a moving target

机译:调节性T细胞抑制机制–移动目标的多样化武器库

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摘要

Naturally-occurring regulatory T cells (Tregs) are emerging as key regulators of immune responses to self-tissues and infectious agents. Insight has been gained into the cell types and the cellular events that are regulated by Tregs. Indeed, Tregs have been implicated in the control of initial activation events, proliferation, differentiation and effector function. However, the mechanisms by which Tregs disable their cellular targets are not well understood. Here we review recent advances in the identification of distinct mechanisms of Treg action and of signals that enable cellular targets to escape regulation. Roles for inhibitory cytokines, cytotoxic molecules, modulators of cAMP and cytokine competition have all been demonstrated. The growing number of inhibitory mechanisms ascribed to Tregs suggests that Tregs take a multi-pronged approach to immune regulation. It is likely that the relative importance of each inhibitory mechanism is context dependent and modulated by the inflammatory milieu and the magnitude of the immune response. In addition, the target cell may be differentially susceptible or resistant to distinct Treg mechanisms depending on their activation or functional status at the time of the Treg encounter. Understanding when and where each suppressive tool is most effective will help to fine tune therapeutic strategies to promote or constrain specific arms of Treg suppression.
机译:天然存在的调节性T细胞(Tregs)逐渐成为对自身组织和传染原免疫反应的关键调节剂。已经了解了由Treg调节的细胞类型和细胞事件。实际上,Treg已经牵涉到对初始活化事件,增殖,分化和效应子功能的控制。但是,Treg禁用其细胞靶标的机制尚不十分清楚。在这里,我们回顾了鉴定Treg作用的独特机制和使细胞靶标能够逃避调控的信号的最新进展。已经证明了抑制性细胞因子,细胞毒性分子,cAMP调节剂和细胞因子竞争的作用。归因于Treg的抑制机制越来越多,这表明Treg对免疫调节采取了多管齐下的方法。每种抑制机制的相对重要性很可能取决于具体情况,并受炎性环境和免疫反应强度的调节。另外,取决于靶细胞在遇到Treg时的激活或功能状态,其可能对不同的Treg机制具有不同的敏感性或抗性。了解每种抑制工具在何时何地最有效,将有助于调整治疗策略,以促进或限制Treg抑制的特定作用。

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