Lagged effects of childhood depressive symptoms on adult epigenetic aging.

IF 5.9 2区 医学 Q1 PSYCHIATRY
Laura K M Han, Moji Aghajani, Brenda W J H Penninx, William E Copeland, Karolina A Aberg, Edwin J C G van den Oord
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引用次数: 0

Abstract

Background: Cross-sectional studies have identified health risks associated with epigenetic aging. However, it is unclear whether these risks make epigenetic clocks 'tick faster' (i.e. accelerate biological aging). The current study examines concurrent and lagged within-person changes of a variety of health risks associated with epigenetic aging.

Methods: Individuals from the Great Smoky Mountains Study were followed from age 9 to 35 years. DNA methylation profiles were assessed from blood, at multiple timepoints (i.e. waves) for each individual. Health risks were psychiatric, lifestyle, and adversity factors. Concurrent (N = 539 individuals; 1029 assessments) and lagged (N = 380 individuals; 760 assessments) analyses were used to determine the link between health risks and epigenetic aging.

Results: Concurrent models showed that BMI (r = 0.15, PFDR < 0.01) was significantly correlated to epigenetic aging at the subject-level but not wave-level. Lagged models demonstrated that depressive symptoms (b = 1.67 months per symptom, PFDR = 0.02) in adolescence accelerated epigenetic aging in adulthood, also when models were fully adjusted for BMI, smoking, and cannabis and alcohol use.

Conclusions: Within-persons, changes in health risks were unaccompanied by concurrent changes in epigenetic aging, suggesting that it is unlikely for risks to immediately 'accelerate' epigenetic aging. However, time lagged analyses indicated that depressive symptoms in childhood/adolescence predicted epigenetic aging in adulthood. Together, findings suggest that age-related biological embedding of depressive symptoms is not instant but provides prognostic opportunities. Repeated measurements and longer follow-up times are needed to examine stable and dynamic contributions of childhood experiences to epigenetic aging across the lifespan.

童年抑郁症状对成年表观遗传衰老的滞后效应。
背景:横断面研究发现了与表观遗传衰老相关的健康风险。然而,目前还不清楚这些风险是否会使表观遗传时钟 "滴答作响"(即加速生物衰老)。本研究探讨了与表观遗传老化相关的各种健康风险在人体内的并发和滞后变化:方法:对 "大烟山研究"(Great Smoky Mountains Study)中的个体进行从 9 岁到 35 岁的跟踪调查。对每个人在多个时间点(即波)的血液中的 DNA 甲基化图谱进行了评估。健康风险包括精神、生活方式和逆境因素。并发(N = 539 人;1029 次评估)和滞后(N = 380 人;760 次评估)分析用于确定健康风险与表观遗传老化之间的联系:并发模型显示,体重指数(r = 0.15,PFDR < 0.01)与表观遗传老化在主体层面有显著相关性,但与波浪层面无关。滞后模型显示,青春期的抑郁症状(b = 1.67 个月/每个症状,PFDR = 0.02)加速了成年期的表观遗传老化,当模型完全调整了体重指数、吸烟、大麻和酒精的使用时也是如此:在人体内,健康风险的变化并不伴随表观遗传衰老的同步变化,这表明风险不太可能立即 "加速 "表观遗传衰老。然而,时滞分析表明,童年/青春期的抑郁症状预示着成年期的表观遗传衰老。综上所述,研究结果表明,与年龄相关的抑郁症状的生物嵌入并非一蹴而就,而是提供了预后机会。要研究童年经历对整个生命周期表观遗传衰老的稳定和动态影响,还需要重复测量和更长的随访时间。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Psychological Medicine
Psychological Medicine 医学-精神病学
CiteScore
11.30
自引率
4.30%
发文量
711
审稿时长
3-6 weeks
期刊介绍: Now in its fifth decade of publication, Psychological Medicine is a leading international journal in the fields of psychiatry, related aspects of psychology and basic sciences. From 2014, there are 16 issues a year, each featuring original articles reporting key research being undertaken worldwide, together with shorter editorials by distinguished scholars and an important book review section. The journal''s success is clearly demonstrated by a consistently high impact factor.
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