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Literature DB >> 30523076

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

Oliver J Harrison¹, Jonathan L Linehan¹, Han-Yu Shih², Nicolas Bouladoux^1,3, Seong-Ji Han¹, Margery Smelkinson⁴, Shurjo K Sen⁵, Allyson L Byrd¹, Michel Enamorado¹, Chen Yao², Samira Tamoutounour¹, Francois Van Laethem⁶, Charlotte Hurabielle^1,7, Nicholas Collins¹, Andrea Paun⁸, Rosalba Salcedo⁹, John J O'Shea², Yasmine Belkaid^10,3.

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.

Entities: Chemical Disease Gene Species

Mesh：

Substances：

Year: 2018 PMID： 30523076 PMCID： PMC7304459 DOI： 10.1126/science.aat6280

Source DB: PubMed Journal: Science ISSN： 0036-8075 Impact factor: 47.728

57 in total

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