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共生特异性 T 细胞可塑性促进组织快速适应损伤。

Commensal-specific T cell plasticity promotes rapid tissue adaptation to injury.

机构信息

Mucosal Immunology Section, Laboratory of Parasitic Diseases, National Institute of Allergy and Infectious Diseases, Bethesda, MD 20892, USA.

Molecular Immunology and Inflammation Branch, National Institute of Arthritis and Musculoskeletal and Skin Diseases, Bethesda, MD 20892, USA.

出版信息

Science. 2019 Jan 4;363(6422). doi: 10.1126/science.aat6280. Epub 2018 Dec 6.

Abstract

Barrier tissues are primary targets of environmental stressors and are home to the largest number of antigen-experienced lymphocytes in the body, including commensal-specific T cells. We found that skin-resident commensal-specific T cells harbor a paradoxical program characterized by a type 17 program associated with a poised type 2 state. Thus, in the context of injury and exposure to inflammatory mediators such as interleukin-18, these cells rapidly release type 2 cytokines, thereby acquiring contextual functions. Such acquisition of a type 2 effector program promotes tissue repair. Aberrant type 2 responses can also be unleashed in the context of local defects in immunoregulation. Thus, commensal-specific T cells co-opt tissue residency and cell-intrinsic flexibility as a means to promote both local immunity and tissue adaptation to injury.

摘要

屏障组织是环境应激源的主要靶标,也是体内经历抗原的最大数量淋巴细胞的所在地,包括共生特异性 T 细胞。我们发现,皮肤驻留的共生特异性 T 细胞具有一种矛盾的程序特征,表现为与准备好的 2 型状态相关的 17 型程序。因此,在受伤和暴露于白细胞介素 18 等炎症介质的情况下,这些细胞迅速释放 2 型细胞因子,从而获得上下文功能。这种获得 2 型效应程序促进组织修复。在免疫调节局部缺陷的情况下,也可能释放异常的 2 型反应。因此,共生特异性 T 细胞利用组织驻留和细胞内在的灵活性作为促进局部免疫和组织适应损伤的手段。

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