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

Mongelli, Alessia; Barbi, Veronica; zamperla, michela gottardi; Atlante, Sandra; Forleo, Luana; Nesta, Marialisa; Massetti, Massimo; Pontecorvi, Alfredo; Nanni, Simona; Farsetti, Antonella; Catalano, Oronzo; Bussotti, Maurizio; Vecchia, Laura Adelaide Dalla; Bachetti, Tiziana; Martelli, Fabio; Rovere, Maria Teresa La; Gaetano, Carlo

doi:10.3390/ijms22116151

Cited by 64 publications

(60 citation statements)

References 51 publications

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“…In fact, it has been demonstrated that HIV infection leads to an average aging advancement of 4.9 years [18]. It has also been suggested that such off-set occurs also if the infection with SARS-CoV-2 has been persistent for a longer time in COVID-19 survivors, particularly in a cohort younger than 60 years [19]. However, blood samples that were taken before a fatal COVID-19 infection were not available, and it appears unlikely that the COVID-19 infection rejuvenates a previously accelerated epigenetic age;…”

Section: Discussionmentioning

confidence: 99%

Epigenetic Clocks Are Not Accelerated in COVID-19 Patients

Franzen

Nüchtern

Tharmapalan

et al. 2021

IJMS

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Age is a major risk factor for severe outcome of the 2019 coronavirus disease (COVID-19). In this study, we followed the hypothesis that particularly patients with accelerated epigenetic age are affected by severe outcomes of COVID-19. We investigated various DNA methylation datasets of blood samples with epigenetic aging signatures and performed targeted bisulfite amplicon sequencing. Overall, epigenetic clocks closely correlated with the chronological age of patients, either with or without acute respiratory distress syndrome. Furthermore, lymphocytes did not reveal significantly accelerated telomere attrition. Thus, these biomarkers cannot reliably predict higher risk for severe COVID-19 infection in elderly patients.

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Section: Discussionmentioning

confidence: 99%

Epigenetic Clocks Are Not Accelerated in COVID-19 Patients

Franzen

Nüchtern

Tharmapalan

et al. 2021

IJMS

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“…Moreover, prior multi-omic analysis has shown that the Levine clock accelerates with cellular senescence and mitochondrial dysfunction (Liu et al, 2020). Prior studies of epigenetic clocks in COVID-19 utilized different sets of clocks which may explain their conflicting results (Corley et al, 2021; Franzen et al, 2021; Mongelli et al, 2021a). Interrogating a wide array of clocks simultaneously is essential for determining which clocks are most related to COVID-19 or vaccination.…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, epigenetic clocks are accurate predictors of mortality risk (Lu et al, 2019), biomarkers of pathogen exposure (Horvath and Levine, 2015; Boulias et al, 2016; Corley et al, 2021), and correlates of lung function and immune inflammation (Hillary et al, 2020, 2021). Evidence suggests that severe COVID-19 disease may impact certain epigenetic clocks (Corley et al, 2021; Mongelli et al, 2021a) and biological aging captured by PhenoAge may inform COVID-19 outcomes (Kuo et al, 2020). More recent epigenetic clock studies have reported conflicting evidence for biological age acceleration and telomere shortening in COVID-19 survivors (Mongelli et al, 2021b), with some finding no clock acceleration in COVID-19 patients (Franzen et al, 2021).…”

Section: Introductionmentioning

confidence: 99%

Longitudinal study of DNA methylation and epigenetic clocks prior to and following test-confirmed COVID-19 and mRNA vaccination

Pang

Higgins‐Chen

Comite

et al. 2021

Preprint

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The host epigenetic landscape is rapidly changed during SARS-CoV-2 infection and evidence suggests that severe COVID-19 is associated with durable scars to the epigenome. Specifically, aberrant DNA methylation changes in immune cells and alterations to epigenetic clocks in blood relate to severe COVID-19. However, a longitudinal assessment of DNA methylation states and epigenetic clocks in blood from healthy individuals prior to and following test-confirmed non-hospitalized COVID-19 has not been performed. Moreover, the impact of mRNA COVID-19 vaccines upon the host epigenome remains understudied. Here, we first examined DNA methylation states in blood of 21 participants prior to and following test confirmed COVID-19 diagnosis at a median timeframe of 8.35 weeks. 261 CpGs were identified as differentially methylated following COVID-19 diagnosis in blood at an FDR adjusted P value <0.05. These CpGs were enriched in gene body and northern and southern shelf regions of genes involved in metabolic pathways. Integrative analysis revealed overlap among genes identified in transcriptional SARS-CoV-2 infection datasets. Principal component-based epigenetic clock estimates of PhenoAge and GrimAge significantly increased in people over 50 following infection by an average of 2.1 and 0.84 years. In contrast, PCPhenoAge significantly decreased in people under 50 following infection by an average of 2.06 years. This observed divergence in epigenetic clocks following COVID-19 was related to age and immune cell-type compositional changes in CD4+ T cells, B cells, granulocytes, plasmablasts, exhausted T cells, and naïve T cells. Complementary longitudinal epigenetic clock analyses of 36 participants prior to and following Pfizer and Moderna mRNA-based COVID-19 vaccination revealed vaccination significantly reduced principal component-based Horvath epigenetic clock estimates in people over 50 by an average of 3.91 years for those that received Moderna. This reduction in epigenetic clock estimates was significantly related to chronological age and immune cell-type compositional changes in B cells and plasmablasts pre- and post-vaccination. These findings suggest the potential utility of epigenetic clocks as a biomarker of COVID-19 vaccine responses. Future research will need to unravel the significance and durability of short-term changes in epigenetic age related to COVID-19 exposure and mRNA vaccination.

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“…Moreover, psychological stress-upregulated ROS trigger telomere attrition, a phenomenon encountered in both PTSD and severe COVID-19, linking these conditions to premature aging (Atanackovic et al, 2002;Yegorov et al, 2020). Interestingly, it was reported that aside from AT-1Rs and ET-1Rs, mitochondria also expressed gamma-aminobutyric acid (GABA), glucocorticoid, and monoamine oxidase A and B receptors, further connecting the organelle to SRDs (Krueger, 1995;Mongelli et al, 2021).…”

Section: Mitochondria and Ptsdmentioning

confidence: 99%

PTSD as an Endothelial Disease: Insights From COVID-19

Sfera

Osorio

Rahman

et al. 2021

Front. Cell. Neurosci.

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Graphical Abstract 1Covid-19 triggers endothelial cell (EC) senescence and dysfunction, likely predisposing to PTSD by increasing microvascular permeability that enables the extravasation of stress molecules into the brain trauma-processing networks in amygdala, hippocampus and the medial prefrontal cortex. The virus upregulates host angiotensin II (ANG II) (via S1 antigen), usurps furin/plasmin (via S2 antigen), mitochondria (via ORF9b), and Sigma-1 receptors (Sig-1Rs) via NSP6. These structures, previously associated with PTSD, link the SARS-CoV-2 virus to increased susceptibility for stress related disorders. As ECs are major producers of brain derived neurotrophic factor (BDNF), a neurotrophin altered in PTSD, senescent ECs lower this molecule further, predisposing to stress related disorders.

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

Cited by 64 publications

References 51 publications

Epigenetic Clocks Are Not Accelerated in COVID-19 Patients

Epigenetic Clocks Are Not Accelerated in COVID-19 Patients

Longitudinal study of DNA methylation and epigenetic clocks prior to and following test-confirmed COVID-19 and mRNA vaccination

PTSD as an Endothelial Disease: Insights From COVID-19

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