Epigenetic age acceleration in surviving versus deceased COVID-19 patients with acute respiratory distress syndrome following hospitalization Journal Article

   


Authors: Bejaoui, Y.; Humaira Amanullah, F.; Saad, M.; Taleb, S.; Bradic, M.; Megarbane, A.; Ait Hssain, A.; Abi Khalil, C.; El Hajj, N.
Article Title: Epigenetic age acceleration in surviving versus deceased COVID-19 patients with acute respiratory distress syndrome following hospitalization
Abstract: Background: Aging has been reported as a major risk factor for severe symptoms and higher mortality rates in COVID-19 patients. Molecular hallmarks such as epigenetic alterations and telomere attenuation reflect the biological process of aging. Epigenetic clocks have been shown to be valuable tools for measuring biological age in various tissues and samples. As such, these epigenetic clocks can determine accelerated biological aging and time-to-mortality across various tissues. Previous reports have shown accelerated biological aging and telomere attrition acceleration following SARS-CoV-2 infection. However, the effect of accelerated epigenetic aging on outcome (death/recovery) in COVID-19 patients with acute respiratory distress syndrome (ARDS) has not been well investigated. Results: In this study, we measured DNA methylation age and telomere attrition in 87 severe COVID-19 cases with ARDS under mechanical ventilation. Furthermore, we compared dynamic changes in epigenetic aging across multiple time points until recovery or death. Epigenetic age was measured using the Horvath, Hannum, DNAm skin and blood, GrimAge, and PhenoAge clocks, whereas telomere length was calculated using the surrogate marker DNAmTL. Our analysis revealed significant accelerated epigenetic aging but no telomere attrition acceleration in severe COVID-19 cases. In addition, we observed epigenetic age deceleration at inclusion versus end of follow-up in recovered but not in deceased COVID-19 cases using certain clocks. When comparing dynamic changes in epigenetic age acceleration (EAA), we detected higher EAA using both the Horvath and PhenoAge clocks in deceased versus recovered patients. The DNAmTL measurements revealed telomere attrition acceleration in deceased COVID-19 patients between inclusion and end of follow-up and a significant change in dynamic telomere attrition acceleration when comparing patients who recovered versus those who died. Conclusions: EAA and telomere attrition acceleration were associated with treatment outcomes in hospitalized COVID-19 patients with ARDS. A better understanding of the long-term effects of EAA in COVID-19 patients and how they might contribute to long COVID symptoms in recovered individuals is urgently needed. © 2023, The Author(s).
Keywords: adult; controlled study; survival analysis; major clinical study; genetics; disease course; outcome assessment; follow up; cohort analysis; dna methylation; intensive care unit; hospitalization; epigenesis, genetic; genetic epigenesis; dna determination; longitudinal study; artificial ventilation; adult respiratory distress syndrome; respiratory distress syndrome; telomere length; acceleration; humans; human; male; female; article; dna methylation age; severe acute respiratory syndrome coronavirus 2; coronavirus disease 2019; covid-19; sars-cov-2; long covid; epigenetic clock; epigenetic age acceleration; epigenetic clocks; post-acute covid-19 syndrome
Journal Title: Clinical Epigenetics
Volume: 15
ISSN: 1868-7075
Publisher: BioMed Central Ltd.  
Date Published: 2023-11-28
Start Page: 186
Language: English
DOI: 10.1186/s13148-023-01597-4
PUBMED: 38017502
PROVIDER: scopus
PMCID: PMC10685564
DOI/URL:

https://www.scopus.com/inward/record.uri?eid=2-s2.0-85178011958&doi=10.1186%2fs13148-023-01597-4&partnerID=40&md5=00aee3041aa4e75262a1b5a51dff2ddb
Notes: Article -- Source: Scopus
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  1. Martina Bradic
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