| Literature DB >> 34283971 |
Christopher B Medina1, Yu-Hsin Chiu2, Marta E Stremska3, Christopher D Lucas4, Ivan Poon5, Kenneth S Tung6, Michael R Elliott1, Bimal Desai7, Ulrike M Lorenz6, Douglas A Bayliss7, Kodi S Ravichandran8.
Abstract
Allergic airway inflammation is driven by type-2 CD4+ T cell inflammatory responses. We uncover an immunoregulatory role for the nucleotide release channel, Panx1, in T cell crosstalk during airway disease. Inverse correlations between Panx1 and asthmatics and our mouse models revealed the necessity, specificity, and sufficiency of Panx1 in T cells to restrict inflammation. Global Panx1-/- mice experienced exacerbated airway inflammation, and T-cell-specific deletion phenocopied Panx1-/- mice. A transgenic designed to re-express Panx1 in T cells reversed disease severity in global Panx1-/- mice. Panx1 activation occurred in pro-inflammatory T effector (Teff) and inhibitory T regulatory (Treg) cells and mediated the extracellular-nucleotide-based Treg-Teff crosstalk required for suppression of Teff cell proliferation. Mechanistic studies identified a Salt-inducible kinase-dependent phosphorylation of Panx1 serine 205 important for channel activation. A genetically targeted mouse expressing non-phosphorylatable Panx1S205A phenocopied the exacerbated inflammation in Panx1-/- mice. These data identify Panx1-dependent Treg:Teff cell communication in restricting airway disease.Entities:
Keywords: Pannexin 1, extracellular ATP, lung, asthma, airway inflammation, T regulatory cell, T effector cell, Salt-inducible kinase, CD4 T cell, adenosine
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Year: 2021 PMID: 34283971 PMCID: PMC8363584 DOI: 10.1016/j.immuni.2021.06.014
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 43.474