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T 细胞激活龛——在炎症和感染组织中优化 T 细胞效应功能。

T cell activation niches-Optimizing T cell effector function in inflamed and infected tissues.

机构信息

Department of Microbiology and Immunology, College of Veterinary Medicine, Cornell University, Ithaca, New York, USA.

出版信息

Immunol Rev. 2022 Mar;306(1):164-180. doi: 10.1111/imr.13047. Epub 2021 Dec 2.

Abstract

Successful immunity to infection, malignancy, and tissue damage requires the coordinated recruitment of numerous immune cell subsets to target tissues. Once within the target tissue, effector T cells rely on local chemotactic cues and structural cues from the tissue matrix to navigate the tissue, interact with antigen-presenting cells, and release effector cytokines. This highly dynamic process has been "caught on camera" in situ by intravital multiphoton imaging. Initial studies revealed a surprising randomness to the pattern of T cell migration through inflamed tissues, behavior thought to facilitate chance encounters with rare antigen-bearing cells. Subsequent tissue-wide visualization has uncovered a high degree of spatial preference when it comes to T cell activation. Here, we discuss the basic tenants of a successful effector T cell activation niche, taking cues from the dynamics of Tfh positioning in the lymph node germinal center. In peripheral tissues, steady-state microanatomical organization may direct the location of "pop-up" de novo activation niches, often observed as perivascular clusters, that support early effector T cell activation. These perivascular activation niches appear to be regulated by site-specific chemokines that coordinate the recruitment of dendritic cells and other innate cells for local T cell activation, survival, and optimized effector function.

摘要

成功抵御感染、恶性肿瘤和组织损伤需要大量免疫细胞亚群的协调募集,以靶向组织。一旦进入靶组织,效应 T 细胞依赖于局部趋化因子线索和组织基质的结构线索来在组织中导航,与抗原呈递细胞相互作用,并释放效应细胞因子。这一高度动态的过程已经通过体内多光子成像“实时”捕捉到。最初的研究揭示了 T 细胞通过炎症组织迁移的模式具有惊人的随机性,这种行为被认为有助于与罕见的抗原呈递细胞偶然相遇。随后的全组织可视化揭示了 T 细胞激活时存在高度的空间偏好。在这里,我们从滤泡辅助性 T 细胞(Tfh)在淋巴结生发中心的定位动力学中得到启示,讨论了成功的效应 T 细胞激活小生境的基本要点。在周围组织中,稳态微解剖结构组织可能会指导“弹出式”新激活小生境的位置,这些小生境通常表现为血管周围簇,支持早期效应 T 细胞的激活。这些血管周围激活小生境似乎受到特定部位趋化因子的调节,这些趋化因子协调树突状细胞和其他先天细胞的募集,以进行局部 T 细胞激活、存活和优化效应功能。

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