| Literature DB >> 29358051 |
Jonathan L Linehan1, Oliver J Harrison1, Seong-Ji Han1, Allyson L Byrd2, Ivan Vujkovic-Cvijin1, Alejandro V Villarino3, Shurjo K Sen4, Jahangheer Shaik5, Margery Smelkinson6, Samira Tamoutounour1, Nicholas Collins1, Nicolas Bouladoux7, Amiran Dzutsev4, Stephan P Rosshart8, Jesse H Arbuckle9, Chyung-Ru Wang10, Thomas M Kristie9, Barbara Rehermann8, Giorgio Trinchieri4, Jason M Brenchley11, John J O'Shea3, Yasmine Belkaid12.
Abstract
Mammalian barrier surfaces are constitutively colonized by numerous microorganisms. We explored how the microbiota was sensed by the immune system and the defining properties of such responses. Here, we show that a skin commensal can induce T cell responses in a manner that is restricted to non-classical MHC class I molecules. These responses are uncoupled from inflammation and highly distinct from pathogen-induced cells. Commensal-specific T cells express a defined gene signature that is characterized by expression of effector genes together with immunoregulatory and tissue-repair signatures. As such, non-classical MHCI-restricted commensal-specific immune responses not only promoted protection to pathogens, but also accelerated skin wound closure. Thus, the microbiota can induce a highly physiological and pleiotropic form of adaptive immunity that couples antimicrobial function with tissue repair. Our work also reveals that non-classical MHC class I molecules, an evolutionarily ancient arm of the immune system, can promote homeostatic immunity to the microbiota. Published by Elsevier Inc.Entities:
Keywords: H2-M3; MHCIb; Staphylococcus epidermidis; microbiota; non-classical MHC class I; skin immunity; tissue repair
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Year: 2018 PMID: 29358051 PMCID: PMC6034182 DOI: 10.1016/j.cell.2017.12.033
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582