DNA methylation age is accelerated in alcohol dependence.

Transl Psychiatry

Section on Clinical Genomics and Experimental Therapeutics, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Bethesda, MD, USA.

Published: September 2018

AI Article Synopsis

  • Alcohol dependence (ALC) is a chronic disorder linked to increased health issues and premature death, and it may affect DNA methylation patterns associated with aging.
  • Researchers studied five different groups to examine the relationship between heavy alcohol use and epigenetic aging using DNA samples from blood, liver, and brain tissue.
  • Findings indicated that certain blood and liver tissue samples from individuals with ALC showed signs of accelerated aging, highlighting the potential for tissue-specific effects of alcohol on epigenetic aging.

Article Abstract

Alcohol dependence (ALC) is a chronic, relapsing disorder that increases the burden of chronic disease and significantly contributes to numerous premature deaths each year. Previous research suggests that chronic, heavy alcohol consumption is associated with differential DNA methylation patterns. In addition, DNA methylation levels at certain CpG sites have been correlated with age. We used an epigenetic clock to investigate the potential role of excessive alcohol consumption in epigenetic aging. We explored this question in five independent cohorts, including DNA methylation data derived from datasets from blood (n = 129, n = 329), liver (n = 92, n = 49), and postmortem prefrontal cortex (n = 46). One blood dataset and one liver tissue dataset of individuals with ALC exhibited positive age acceleration (p < 0.0001 and p = 0.0069, respectively), whereas the other blood and liver tissue datasets both exhibited trends of positive age acceleration that were not significant (p = 0.83 and p = 0.57, respectively). Prefrontal cortex tissue exhibited a trend of negative age acceleration (p = 0.19). These results suggest that excessive alcohol consumption may be associated with epigenetic aging in a tissue-specific manner and warrants further investigation using multiple tissue samples from the same individuals.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6125381PMC
http://dx.doi.org/10.1038/s41398-018-0233-4DOI Listing

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