Mitochondrial DNA Copy Number Variation in Asthma Risk, Severity, and Exacerbations

Although airway oxidative stress and inflammation are central to asthma pathogenesis, there is limited knowledge of the relationship of asthma risk, severity, or exacerbations to mitochondrial dysfunction, which is pivotal to oxidant generation and inflammation. We investigated whether mitochondrial...

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Published inmedRxiv : the preprint server for health sciences
Main Authors Xu, Weiling, Hong, Yun Soo, Hu, Bo, Comhair, Suzy A A, Janocha, Allison J, Zein, Joe G, Chen, Ruoying, Meyers, Deborah A, Mauger, David T, Ortega, Victor E, Bleecker, Eugene R, Castro, Mario, Denlinger, Loren C, Fahy, John V, Israel, Elliot, Levy, Bruce D, Jarjour, Nizar N, Moore, Wendy C, Wenzel, Sally E, Gaston, Benjamin, Liu, Chunyu, Arking, Dan E, Erzurum, Serpil C
Format Journal Article
LanguageEnglish
Published United States 05.12.2023
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Summary:Although airway oxidative stress and inflammation are central to asthma pathogenesis, there is limited knowledge of the relationship of asthma risk, severity, or exacerbations to mitochondrial dysfunction, which is pivotal to oxidant generation and inflammation. We investigated whether mitochondrial DNA copy number (mtDNA-CN) as a measure of mitochondrial function is associated with asthma diagnosis, severity, oxidative stress, and exacerbations. We measured mtDNA-CN in blood in two cohorts. In the UK Biobank (UKB), we compared mtDNA-CN in mild and moderate-severe asthmatics to non-asthmatics. In the Severe Asthma Research Program (SARP), we evaluated mtDNA-CN in relation to asthma severity, biomarkers of oxidative stress and inflammation, and exacerbations. In UK Biobank, asthmatics ( = 29,768) have lower mtDNA-CN compared to non-asthmatics ( = 239,158) (beta, -0.026 [95% CI, -0.038 to -0.014], = 2.46×10 ). While lower mtDNA-CN is associated with asthma, mtDNA-CN did not differ by asthma severity in either UKB or SARP. Biomarkers of inflammation show that asthmatics have higher white blood cells (WBC), neutrophils, eosinophils, fraction exhaled nitric oxide (F NO), and lower superoxide dismutase (SOD) than non-asthmatics, confirming greater oxidative stress in asthma. In one year follow-up in SARP, higher mtDNA-CN is associated with reduced risk of three or more exacerbations in the subsequent year (OR 0.352 [95% CI, 0.164 to 0.753], = 0.007). Asthma is characterized by mitochondrial dysfunction. Higher mtDNA-CN identifies an exacerbation-resistant asthma phenotype, suggesting mitochondrial function is important in exacerbation risk.