| Literature DB >> 31437129 |
Matthew C Altman1, Ying Lai2, James D Nolin2, Sydney Long1, Chien-Chang Chen2, Adrian M Piliponsky3, William A Altemeier2, Megan Larmore4, Charles W Frevert4, Michael S Mulligan5, Steven F Ziegler6, Jason S Debley3,7, Michael C Peters8, Teal S Hallstrand2.
Abstract
Asthma is a heterogeneous syndrome that has been subdivided into physiologic phenotypes and molecular endotypes. The most specific phenotypic manifestation of asthma is indirect airway hyperresponsiveness (AHR), and a prominent molecular endotype is the presence of type 2 inflammation. The underlying basis for type 2 inflammation and its relationship to AHR are incompletely understood. We assessed the expression of type 2 cytokines in the airways of subjects with and without asthma who were extensively characterized for AHR. Using quantitative morphometry of the airway wall, we identified a shift in mast cells from the submucosa to the airway epithelium specifically associated with both type 2 inflammation and indirect AHR. Using ex vivo modeling of primary airway epithelial cells in organotypic coculture with mast cells, we show that epithelial-derived IL-33 uniquely induced type 2 cytokines in mast cells, which regulated the expression of epithelial IL33 in a feed-forward loop. This feed-forward loop was accentuated in epithelial cells derived from subjects with asthma. These results demonstrate that type 2 inflammation and indirect AHR in asthma are related to a shift in mast cell infiltration to the airway epithelium, and that mast cells cooperate with epithelial cells through IL-33 signaling to regulate type 2 inflammation.Entities:
Keywords: Asthma; Immunology; Mast cells; Pulmonology; Th2 response
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Year: 2019 PMID: 31437129 PMCID: PMC6819127 DOI: 10.1172/JCI126402
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808