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IL-13Rα2 and IL-10 coordinately suppress airway inflammation, airway-hyperreactivity, and fibrosis in mice
Mark S. Wilson, … , Allen W. Cheever, Thomas A. Wynn
Mark S. Wilson, … , Allen W. Cheever, Thomas A. Wynn
Published October 1, 2007
Citation Information: J Clin Invest. 2007;117(10):2941-2951. https://doi.org/10.1172/JCI31546.
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Research Article Immunology

IL-13Rα2 and IL-10 coordinately suppress airway inflammation, airway-hyperreactivity, and fibrosis in mice

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Abstract

Development of persistent Th2 responses in asthma and chronic helminth infections are a major health concern. IL-10 has been identified as a critical regulator of Th2 immunity, but mechanisms for controlling Th2 effector function remain unclear. IL-10 also has paradoxical effects on Th2-associated pathology, with IL-10 deficiency resulting in increased Th2-driven inflammation but also reduced airway hyperreactivity (AHR), mucus hypersecretion, and fibrosis. We demonstrate that increased IL-13 receptor α 2 (IL-13Rα2) expression is responsible for the reduced AHR, mucus production, and fibrosis in BALB/c IL-10–/– mice. Using models of allergic asthma and chronic helminth infection, we demonstrate that IL-10 and IL-13Rα2 coordinately suppress Th2-mediated inflammation and pathology, respectively. Although IL-10 was identified as the dominant antiinflammatory mediator, studies with double IL-10/IL-13Rα2–deficient mice illustrate an indispensable role for IL-13Rα2 in the suppression of AHR, mucus production, and fibrosis. Thus, IL-10 and IL-13Rα2 are both required to control chronic Th2-driven pathological responses.

Authors

Mark S. Wilson, Eldad Elnekave, Margaret M. Mentink-Kane, Marcus G. Hodges, John T. Pesce, Thirumalai R. Ramalingam, Robert W. Thompson, Masahito Kamanaka, Richard A. Flavell, Andrea Keane-Myers, Allen W. Cheever, Thomas A. Wynn

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Figure 8

Increased granuloma volume and fibrosis in IL-10–/–IL-13Rα2–/– dKO mice.

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Increased granuloma volume and fibrosis in IL-10–/–IL-13Rα2–/– dKO mice....
Mice were infected with 30 S. mansoni cercariae and euthanized at week 8 (early) and week 12 (late) during the chronic stages of egg-induced pathology. *P < 0.05, Mann-Whitney U test for single comparisons or 1-way ANOVA for multiple comparisons. Similar numbers of paired adult parasites and eggs were found in the tissues of all groups, so the observed pathological changes were not attributed to differences in parasite burden. (A) Liver tissue was excised, fixed, sectioned, and stained with Wright-Giemsa. Granuloma volume was calculated in a blinded fashion from Giemsa-stained liver sections at weeks 8 (left) and 12 (right) after infection. (B) Liver fibrosis (μmol of hydroxyproline per worm pair) was calculated from liver biopsies taken at weeks 8 (left) and 12 (right) after infection. (C) A survival study was conducted with mice infected with 30 S. mansoni cercariae.

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ISSN: 0021-9738 (print), 1558-8238 (online)

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