客观和主观的睡眠起始测量指标与青少年的 DNA 甲基化呈不同相关。
Objective and subjective measures of sleep initiation are differentially associated with DNA methylation in adolescents.
机构信息
Sleep Research and Treatment Center, Department of Psychiatry & Behavioral Health, The Pennsylvania State University College of Medicine, Hershey, PA, 17033, USA.
Department of Public Health Sciences, The Pennsylvania State University College of Medicine, Hershey, PA, 17033, USA.
出版信息
Clin Epigenetics. 2023 Aug 26;15(1):136. doi: 10.1186/s13148-023-01553-2.
INTRODUCTION
The onset of puberty is associated with a shift in the circadian timing of sleep, leading to delayed sleep initiation [i.e., later sleep onset time (SOT)] due to later bedtimes and/or longer sleep onset latency (SOL). Several genome-wide association studies (GWAS) have identified genes that may be involved in the etiology of sleep phenotypes. However, circadian rhythms are also epigenetically regulated; therefore, epigenetic biomarkers may provide insight into the physiology of the pubertal sleep onset shift and the pathophysiology of prolonged or delayed sleep initiation.
RESULTS
The gene-wide analysis indicated differential methylation within or around 1818 unique genes across the sleep initiation measurements using self-report, actigraphy (ACT), and polysomnography (PSG), while GWAS-informed analysis yielded 67 genes. Gene hits were identified for bedtime (PSG), SOL (subjective, ACT and PSG) and SOT (subjective and PSG). DNA methylation within 12 genes was associated with both subjective and PSG-measured SOL, 31 with both ACT- and PSG-measured SOL, 19 with both subjective and ACT-measured SOL, and one gene (SMG1P2) had methylation sites associated with subjective, ACT- and PSG-measured SOL.
CONCLUSIONS
Objective and subjective sleep initiation in adolescents is associated with altered DNA methylation in genes previously identified in adult GWAS of sleep and circadian phenotypes. Additionally, our data provide evidence for a potential epigenetic link between habitual (subjective and ACT) SOL and in-lab SOT and DNA methylation in and around genes involved in circadian regulation (i.e., RASD1, RAI1), cardiometabolic disorders (i.e., FADS1, WNK1, SLC5A6), and neuropsychiatric disorders (i.e., PRR7, SDK1, FAM172A). If validated, these sites may provide valuable targets for early detection and prevention of disorders involving prolonged or delayed SOT, such as insomnia, delayed sleep phase, and their comorbidity.
简介
青春期的开始与睡眠的昼夜节律时间变化有关,导致入睡时间延迟[即,较晚的上床时间和/或更长的入睡潜伏期 (SOL)]。几项全基因组关联研究 (GWAS) 已经确定了可能与睡眠表型病因有关的基因。然而,昼夜节律也受到表观遗传调控;因此,表观遗传生物标志物可以深入了解青春期睡眠起始变化的生理学和延长或延迟入睡起始的病理生理学。
结果
全基因分析表明,在使用自我报告、活动记录仪 (ACT) 和多导睡眠图 (PSG) 测量睡眠起始时,在 1818 个独特基因的内部或周围存在差异甲基化,而 GWAS 知情分析产生了 67 个基因。基因命中与上床时间 (PSG)、SOL (主观、ACT 和 PSG) 和 SOT (主观和 PSG) 有关。12 个基因内的 DNA 甲基化与主观和 PSG 测量的 SOL 均有关,31 个与 ACT 和 PSG 测量的 SOL 均有关,19 个与主观和 ACT 测量的 SOL 均有关,一个基因 (SMG1P2) 有与主观、ACT 和 PSG 测量的 SOL 有关的甲基化位点。
结论
青少年的客观和主观睡眠起始与先前在成人睡眠和昼夜节律表型 GWAS 中确定的基因的 DNA 甲基化改变有关。此外,我们的数据提供了证据表明习惯性(主观和 ACT)SOL 与实验室内 SOT 之间以及昼夜节律调节基因(即 RASD1、RAI1)、心脏代谢紊乱(即 FADS1、WNK1、SLC5A6)和神经精神障碍(即 PRR7、SDK1、FAM172A)中基因的 DNA 甲基化之间存在潜在的表观遗传联系。如果得到验证,这些位点可能为检测和预防涉及延长或延迟 SOT 的疾病提供有价值的靶点,例如失眠、睡眠阶段延迟及其共病。
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