A distinctive DNA methylation pattern in insufficient sleep

Authors :: Perttu Salo
Alexandra Lahtinen
Natalia Pervjakova
Päivi Vanttola
Sonja Sulkava
Mikko Härmä
Markus Perola
Sampsa Puttonen
Lili Milani
Tiina Paunio
Katriina Viitasalo
Auli Toivola
Anni Joensuu
Department of Psychiatry
University of Helsinki
Clinicum
HUS Psychiatry
Quantitative Genetics
Diabetes and Obesity Research Program
Research Programs Unit
Tampere University
Source :: Scientific Reports, Vol 9, Iss 1, Pp 1-9 (2019), Scientific Reports
Publication Year :: 2019
Publisher :: Springer Science and Business Media LLC, 2019.
Abstract: Short sleep duration or insomnia may lead to an increased risk of various psychiatric and cardio-metabolic conditions. Since DNA methylation plays a critical role in the regulation of gene expression, studies of differentially methylated positions (DMPs) might be valuable for understanding the mechanisms underlying insomnia. We performed a cross-sectional genome-wide analysis of DNA methylation in relation to self-reported insufficient sleep in individuals from a community-based sample (79 men, aged 39.3 ± 7.3), and in relation to shift work disorder in an occupational cohort (26 men, aged 44.9 ± 9.0). The analysis of DNA methylation data revealed that genes corresponding to selected DMPs form a distinctive pathway: “Nervous System Development” (FDR P value