Igor Santiago-Carvalho, Alma Banuelos, Henrique Borges da Silva
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引用次数: 0
Abstract
The activation and function of T cells is fundamental for the control of infectious diseases and cancer, and conversely can mediate several autoimmune diseases. Among the signaling pathways leading to T cell activation and function, the sensing of extracellular adenosine triphosphate (eATP) has been recently appreciated as an important component. Through a plethora of purinergic receptors, most prominently P2RX7, eATP sensing can induce a wide variety of processes in T cells, such as proliferation, subset differentiation, survival, or cell death. The downstream roles of eATP sensing can vary according to (a) the T cell subset, (b) the tissue where T cells are, and (c) the time after antigen exposure. In this mini-review, we revisit the recent findings on how eATP signaling pathways regulate T-cell immune responses and posit important unanswered questions on this field.
T 细胞的活化和功能是控制传染病和癌症的基础,反之也可介导多种自身免疫性疾病。在导致 T 细胞活化和发挥功能的信号通路中,对细胞外三磷酸腺苷(eATP)的感应最近被认为是一个重要的组成部分。通过大量嘌呤能受体(最主要的是 P2RX7),eATP 可诱导 T 细胞的各种过程,如增殖、亚群分化、存活或细胞死亡。eATP 传感的下游作用会因(a)T 细胞亚群、(b)T 细胞所在的组织以及(c)抗原暴露后的时间而有所不同。在这篇微型综述中,我们将重温有关 eATP 信号通路如何调控 T 细胞免疫反应的最新发现,并提出这一领域的重要未解之谜。