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A Transcriptomic Method to Determine Airway Immune Dysfunction in T2-High and T2-Low Asthma

医学 免疫学 免疫系统 哮喘 炎症 先天免疫系统 病理 肺结核
作者
Michael C. Peters,Lando Ringel,Nathan Dyjack,Rachelle Herrin,Prescott G. Woodruff,Cydney Rios,Brian D. O’Connor,John V. Fahy,Max A. Seibold
出处
期刊:American Journal of Respiratory and Critical Care Medicine [American Thoracic Society]
卷期号:199 (4): 465-477 被引量:150
标识
DOI:10.1164/rccm.201807-1291oc
摘要

Abstract Background Type 2 (T2) inflammation drives airway dysfunction in many patients with asthma; yet, we lack a comprehensive understanding of the airway immune cell types and networks that sustain this inflammation. Moreover, defects in the airway immune system in patients with asthma without T2 inflammation are not established. Objectives To determine the gene networks that sustain T2 airway inflammation in T2-high asthma and to explore the gene networks that characterize T2-low asthma. Methods Network analysis of sputum cell transcriptome expression data from 84 subjects with asthma and 27 healthy control subjects was used to identify immune cell type–enriched networks that underlie asthma subgroups. Results Sputum T2 gene expression was characterized by an immune cell network derived from multiple innate immune cells, including eosinophils, mast cells/basophils, and inflammatory dendritic cells. Clustering of subjects within this network stratified subjects into T2-high and T2-low groups, but it also revealed a subgroup of T2-high subjects with uniformly higher expression of the T2 network. These “T2-ultrahigh subjects” were characterized clinically by older age and more severe airflow obstruction and pathologically by a second T2 network derived from T2-skewed, CD11b+/CD103−/IRF4+ classical dendritic cells. Subjects with T2-low asthma were differentiated from healthy control subjects by lower expression of a cytotoxic CD8+ T-cell network, which was negatively correlated with body mass index and plasma IL-6 concentrations. Conclusions Persistent airway T2 inflammation is a complex construct of innate and adaptive immunity gene expression networks that are variable across individuals with asthma and persist despite steroid treatment. Individuals with T2-low asthma exhibit an airway deficiency in cytotoxic T cells associated with obesity-driven inflammation.
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