Lung CD103+ dendritic cells restrain allergic airway inflammation through IL-12 production
Laura Conejero, Sofía C. Khouili, Sarai Martínez-Cano, Helena M. Izquierdo, Paola Brandi, David Sancho
Laura Conejero, Sofía C. Khouili, Sarai Martínez-Cano, Helena M. Izquierdo, Paola Brandi, David Sancho
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Research Article Immunology Inflammation

Lung CD103+ dendritic cells restrain allergic airway inflammation through IL-12 production

Abstract

DCs are necessary and sufficient for induction of allergic airway inflammation. CD11b+ DCs direct the underlying Th2 immunity, but debate surrounds the function of CD103+ DCs in lung immunity and asthma after an allergic challenge. We challenged Batf3–/– mice, which lacked lung CD103+ DCs, with the relevant allergen house dust mite (HDM) as a model to ascertain their role in asthma. We show that acute and chronic HDM exposure leads to defective Th1 immunity in Batf3-deficient mice. In addition, chronic HDM challenge in Batf3–/– mice results in increased Th2 and Th17 immune responses and exacerbated airway inflammation. Mechanistically, Batf3 absence does not affect induction of Treg or IL-10 production by lung CD4+ T cells following acute HDM challenge. Batf3-dependent CD103+ migratory DCs are the main source of IL-12p40 in the mediastinal lymph node DC compartment in the steady state. Moreover, CD103+ DCs selectively increase their IL-12p40 production upon HDM administration. In vivo IL-12 treatment reverts exacerbated allergic airway inflammation upon chronic HDM challenge in Batf3–/– mice, restraining Th2 and Th17 responses without triggering Th1 immunity. These results suggest a protective role for lung CD103+ DCs to HDM allergic airway inflammation through the production of IL-12.

Authors

Laura Conejero, Sofía C. Khouili, Sarai Martínez-Cano, Helena M. Izquierdo, Paola Brandi, David Sancho

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Figure 4

Batf3–/– mice develop exacerbated HDM-induced chronic airway inflammation.

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Batf3–/– mice develop exacerbated HDM-induced chronic airway inflammati...
(A) Schematic regime of chronic HDM exposure. (B) Inflammatory infiltrates in BAL from the indicated treatments and genotypes (n = 3 PBS, n = 7 HDM). (C) Representative histological staining of mice of the indicated genotype chronically exposed to HDM. Top: H&E staining (arrowheads point at perivascular and peribronchial infiltration) and PAS staining (insets depict mucus-producing goblet cells). Bottom: staining for collagen (Sirius red). Scale bars: 200 μm (PAS-PBS or H&E) or 100 μm (PAS-HDM or Sirius red). Right: inflammation score (n = 5 PBS, 9 HDM). (D–F) Total serum IgE (D) and HDM-specific IgG2a (E) and IgG1 (F) (n = 5 PBS, n = 10 HDM). (B–F) Individual data and mean ± SEM from 1 experiment representative of at least 3 independent experiments; *P < 0.05, **P < 0.01, ***P < 0.001, Mann Whitney U test. HDM, house dust mite; PAS, periodic acid Schiff.