4.7 Article

Evidence for Biological Age Acceleration and Telomere Shortening in COVID-19 Survivors

期刊

出版社

MDPI
DOI: 10.3390/ijms22116151

关键词

biological age; COVID-19; post-COVID-19; telomeres; epigenetics; DNA methylation; ACE2; DPP-4; DeltaAge

资金

  1. ITALIAN MINISTRY OF EDUCATION, UNIVERSITY AND RESEARCH [PRIN2017S55RXB, PRIN2015HPMLFY]
  2. ITALIAN MINISTRY OF HEALTH [2010-2318330]
  3. Progetto di Rete Cardiovascolare IRCCS: CardioCovid
  4. progetto di rete Aging IRCCS: progetto IRMA e progetto SIRI
  5. Italian Ministry of Health
  6. Telethon Foundation [446 GGP19035A]
  7. AFM-Telethon [23054]
  8. EU Horizon 2020 project COVIRNA [101016072]
  9. ASSOCIAZIONE ITALIANA PER LA RICERCA SUL CANCRO AIRC under IG 2019 [22858]
  10. EU-CardioRNA COST Action [CA17129]

向作者/读者索取更多资源

COVID-19 infection leads to a range of severe sequelae, including a significant increase in biological age and telomere shortening. These sequelae are particularly pronounced in younger patients.
The SARS-CoV-2 infection determines the COVID-19 syndrome characterized, in the worst cases, by severe respiratory distress, pulmonary and cardiac fibrosis, inflammatory cytokine release, and immunosuppression. This condition has led to the death of about 2.15% of the total infected world population so far. Among survivors, the presence of the so-called persistent post-COVID-19 syndrome (PPCS) is a common finding. In COVID-19 survivors, PPCS presents one or more symptoms: fatigue, dyspnea, memory loss, sleep disorders, and difficulty concentrating. In this study, a cohort of 117 COVID-19 survivors (post-COVID-19) and 144 non-infected volunteers (COVID-19-free) was analyzed using pyrosequencing of defined CpG islands previously identified as suitable for biological age determination. The results show a consistent biological age increase in the post-COVID-19 population, determining a DeltaAge acceleration of 10.45 +/- 7.29 years (+5.25 years above the range of normality) compared with 3.68 +/- 8.17 years for the COVID-19-free population (p < 0.0001). A significant telomere shortening parallels this finding in the post-COVID-19 cohort compared with COVID-19-free subjects (p < 0.0001). Additionally, ACE2 expression was decreased in post-COVID-19 patients, compared with the COVID-19-free population, while DPP-4 did not change. In light of these observations, we hypothesize that some epigenetic alterations are associated with the post-COVID-19 condition, particularly in younger patients (< 60 years).

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