BMC Research Notes (Sep 2019)

A pilot prospective study of sleep patterns and DNA methylation-characterized epigenetic aging in young adults

  • Mary A. Carskadon,
  • Kenneth R. Chappell,
  • David H. Barker,
  • Anne C. Hart,
  • Kayla Dwyer,
  • Caroline Gredvig-Ardito,
  • Caitlyn Starr,
  • John E. McGeary

DOI
https://doi.org/10.1186/s13104-019-4633-1
Journal volume & issue
Vol. 12, no. 1
pp. 1 – 5

Abstract

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Abstract Objective Molecular markers in DNA methylation at a subset of CpG sites are affected by the environment and contribute to biological (epigenetic) age. We hypothesized that shorter sleep duration and possibly irregular sleep would be associated with accelerated epigenetic aging. We examined epigenetic vs. chronological age in 12 young women selected as shorter or longer sleepers studied prospectively across the first 9 weeks of college using a daily online sleep log. Genomic DNA was isolated from two blood samples spanning the interval, and DNA methylation levels were determined and used to measure epigenetic age. Results Epigenetic vs. chronological age differences averaged 2.07 at Time 1 and 1.21 at Time 2. Sleep duration was computed as average daily total sleep time and sleep regularity was indexed using the Sleep Regularity Index. Participants with longer and more regular sleep showed reduced age difference: mean = − 2.48 [95% CI − 6.11; 1.15]; those with shorter and more irregular sleep showed an increased age difference: 3.03 [0.02; 6.03]; and those with either shorter or more irregular sleep averaged no significant change: − 0.49 [− 3.55; 2.56]. These pilot data suggest that short and irregular sleep, even in a young healthy sample, may be associated with accelerated epigenetic aging.

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