Journal
ALLERGY
Volume 74, Issue 5, Pages 933-943Publisher
WILEY
DOI: 10.1111/all.13679
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BackgroundWe previously showed that patients with severe allergic asthma have high numbers of circulating ILC2s expressing CCR10. MethodHerein, CCR10(+) ILC2s were further analyzed in the blood of healthy individuals or patients with allergic and non-allergic asthma. Characteristics of human CCR10(+) and CCR10(-) ILC2s were assessed by flow cytometry as well as single-cell multiplex RT-qPCR. The role of CCR10(+) ILC2s in asthma pathophysiology was studied in allergen-treated mice. ResultsWhen compared to healthy controls, CCR10(+) ILC2s are enriched in the blood of both allergic and non-allergic severe asthmatic patients, and these cells are recruited to the lungs. Plasma concentrations of the CCR10 ligand CCL27 are significantly increased in severe asthmatics when compared to non-asthmatic patients. CCR10(+) ILC2s secrete little T(H)2 cytokines, but exhibit ILC1-like properties, including a capacity to produce IFN-. Also, single-cell analysis reveals that the CCR10(+) ILC2 subset is enriched in cells expressing amphiregulin. CCR10(+) ILC2 depletion, as well as blocking of IFN- activity, exacerbates airway hyperreactivity in allergen-challenged mice, providing evidence for a protective role of these cells in allergic inflammation. ConclusionsFrequencies of circulating CCR10(+) ILC2s and CCL27 plasma concentrations represent candidate markers of asthma severity. The characterization of CCR10(+) ILC2s in human samples and in mouse asthma models suggests that these cells downregulate allergic inflammation through IFN- production.
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