David W Sosnowski, Emily J Smail, Brion S Maher, Ann Zenobia Moore, Pei-Lun Kuo, Mark N Wu, Dominique V Low, Katie L Stone, Eleanor M Simonsick, Luigi Ferrucci, Adam P Spira
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引用次数: 0
摘要
我们试图探讨睡眠时间短的遗传风险和自我报告的睡眠时间短是否与生物衰老有关,以及年龄和性别是否会缓和这些关联。参与者是巴尔的摩老龄化纵向研究(Baltimore Longitudinal Study of Aging)中的一部分人,他们拥有完整的自我报告睡眠数据(567 人)或基因型数据(367 人)。结果包括内在 Horvath 年龄、Hannum 年龄、PhenoAge、GrimAge 以及基于 DNAm 的纤溶酶原激活物抑制剂-1(PAI-1)和粒细胞计数估计值。结果表明,短时睡眠的多基因风险与粒细胞计数呈正相关;与报告 7 小时睡眠的人相比,PhenoAge 和 GrimAge 加速更快,估计的 PAI-1 值更高。睡眠时间短的多基因风险和自我报告的睡眠时间与年龄和性别在某些结果上存在相互作用。研究结果突出表明,睡眠时间短的多基因风险和自我报告的睡眠时间长与表观遗传景观的变化以及随后的衰老有关。
Sleep Duration Polygenic Risk and Phenotype: Associations with Biomarkers of Accelerated Aging in the Baltimore Longitudinal Study of Aging.
We sought to explore whether genetic risk for, and self-reported, short sleep are associated with biological aging and whether age and sex moderate these associations. Participants were a subset of individuals from the Baltimore Longitudinal Study of Aging who had complete data on self-reported sleep (n = 567) or genotype (n = 367). Outcomes included: Intrinsic Horvath age, Hannum age, PhenoAge, GrimAge, and DNAm-based estimates of plasminogen activator inhibitor-1 (PAI-1) and granulocyte count. Results demonstrated that polygenic risk for short sleep was positively associated with granulocyte count; compared to those reporting <6 hr sleep, those reporting >7 hr demonstrated faster PhenoAge and GrimAge acceleration and higher estimated PAI-1. Polygenic risk for short sleep and self-reported sleep duration interacted with age and sex in their associations with some of the outcomes. Findings highlight that polygenic risk for short sleep and self-reported long sleep is associated with variation in the epigenetic landscape and subsequently aging.
期刊介绍:
These are some of the broad questions with which the International Journal of Aging and Human Development is concerned. Emphasis is upon psychological and social studies of aging and the aged. However, the Journal also publishes research that introduces observations from other fields that illuminate the "human" side of gerontology, or utilizes gerontological observations to illuminate in other fields.