A neutrophil/TGF-β axis limits the pathogenicity of allergen-specific CD4+ T cells
Gregory S. Whitehead, Seddon Y. Thomas, Keiko Nakano, Derek J. Royer, Catherine G. Burke, Hideki Nakano, Donald N. Cook
Gregory S. Whitehead, Seddon Y. Thomas, Keiko Nakano, Derek J. Royer, Catherine G. Burke, Hideki Nakano, Donald N. Cook
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Research Article Immunology Inflammation

A neutrophil/TGF-β axis limits the pathogenicity of allergen-specific CD4+ T cells

Abstract

The intensity and longevity of inflammatory responses to inhaled allergens is determined largely by the balance between effector and regulatory immune responses, but the mechanisms that determine the relative magnitudes of these opposing forces remain poorly understood. We have found that the type of adjuvant used during allergic sensitization has a profound effect on both the nature and longevity of the pulmonary inflammation triggered by subsequent reexposure to that same provoking allergen. TLR ligand adjuvants and house dust extracts primed immune responses characterized by a mixed neutrophilic and eosinophilic inflammation that was suppressed by multiple daily allergen challenges. During TLR ligand–mediated allergic sensitization, mice displayed transient airway neutrophilia, which triggered the release of TGF-β into the airway. This neutrophil-dependent production of TGF-β during sensitization had a delayed, suppressive effect on eosinophilic responses to subsequent allergen challenge. Neutrophil depletion during sensitization did not affect numbers of Foxp3+ Tregs but increased proportions of Gata3+CD4+ T cells, which, upon their transfer to recipient mice, triggered stronger eosinophilic inflammation. Thus, a neutrophil/TGF-β axis acts during TLR-mediated allergic sensitization to fine-tune the phenotype of developing allergen-specific CD4+ T cells and limit their pathogenicity, suggesting a novel immunotherapeutic approach to control eosinophilia in asthma.

Authors

Gregory S. Whitehead, Seddon Y. Thomas, Keiko Nakano, Derek J. Royer, Catherine G. Burke, Hideki Nakano, Donald N. Cook

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Figure 1

The nature and longevity of allergic responses depend on the type of adjuvant used during sensitization.

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The nature and longevity of allergic responses depend on the type of adj...
(A and B) Mice were sensitized to OVA using either Aspergillus oryzae (ASP) or LPS as the adjuvant, then challenged on a single occasion with aerosolized OVA. (A) Timeline of allergic sensitizations, single challenge, and harvest. (B) Percentages of Th2 (Gata3+) cells, Th17 (RORγt+) cells, and Tregs (Foxp3+CD25+) in CD4+ T cells from lungs of mice 2 days after a single challenge. (n = 6 mice/group). (C) Timeline of sensitizations, daily challenges, and harvest. (D) Airway inflammation 1 day after the last of the indicated number of OVA challenges (n = 5 mice/group). (E) Airway hyperresponsiveness (AHR) measured 2 days after a single challenge or 1 day after the last of 7 daily challenges (n = 6 mice/group). Data shown represent mean values ± SEM from a single experiment, representative of 2, except for B, a single experiment. *P < 0.05; **P < 0.01; ***P < 0.001; unchallenged (0) group vs. allergen-challenged groups; Kruskal-Wallis 1-way ANOVA with Dunn’s multiple-comparison test. R, resistance; MCH, methacholine.