研究健康行为是青春期提前与青春后期表观遗传衰老加速之间的联系机制。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Marlon Goering, Hemant K Tiwari, Amit Patki, Carlos N Espinoza, David C Knight, Sylvie Mrug
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引用次数: 0

摘要

青春期提前与表观遗传衰老加速有关,但其潜在机制尚不清楚。这项三波纵向研究考察了负面健康行为,特别是青春期中期的药物使用、睡眠时间短和饮食质量差,这些行为是青春期早期表型和感知青春期时间提前与青春期晚期三个表观遗传时钟(GrimAge、DunedinPACE 和 PhenoAge)上的表观遗传衰老之间联系的中介因素。表型青春期时间测量的是相对于计时年龄的身体青春期成熟度,而感知青春期时间则是基于青少年对自己相对于同龄人的青春期时间的主观解释。参与者包括 1213 名青少年(51% 女性,49% 男性;62% 黑人,34% 白人),他们分别在青春期早期(平均年龄为 13.10 岁)、青春期中期(平均年龄为 16.1 岁)和青春期晚期(平均年龄为 19.7 岁)参加了研究。中介模型的结果表明,青春期表型时间提前对青春期晚期的 GrimAge 加速有中介效应,因为青春期中期的药物使用率较高。表型青春期时间提前对男性达尼丁青春期加速也有直接影响。睡眠时间和饮食质量并没有成为中介因素,但较短的睡眠时间可预测女性的 GrimAge 加速。这些研究结果表明,较高的药物使用率是早熟青少年经历较快表观遗传衰老的一种机制,这种衰老使他们在整个生命周期中面临健康状况较差的风险。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Examining Health Behaviors as Mechanisms Linking Earlier Pubertal Timing with Accelerated Epigenetic Aging in Late Adolescence.

Examining Health Behaviors as Mechanisms Linking Earlier Pubertal Timing with Accelerated Epigenetic Aging in Late Adolescence.

Earlier pubertal timing is associated with accelerated epigenetic aging, but the underlying mechanisms are not well understood. This three-wave longitudinal study examined negative health behaviors, specifically substance use, short sleep duration, and poor diet quality in middle adolescence, as mediators of links between earlier phenotypic and perceived pubertal timing measured in early adolescence and epigenetic aging on three epigenetic clocks in late adolescence (GrimAge, DunedinPACE, and PhenoAge). Phenotypic pubertal timing measured physical pubertal maturation relative to chronological age, whereas perceived pubertal timing was based on adolescents' subjective interpretation of their pubertal timing relative to their peers. Participants included 1213 youth (51% female, 49% male; 62% Black, 34% White) who participated during early adolescence (mean age = 13.10 years), middle adolescence (mean age = 16.1 years) and late adolescence (mean age = 19.7 years). Results from a mediation model revealed a mediation effect of earlier phenotypic pubertal timing on accelerated GrimAge in late adolescence through higher substance use during middle adolescence. There was also a direct effect of earlier phenotypic pubertal timing on accelerated DunedinPACE in males. Sleep duration and diet quality did not emerge as mediators but shorter sleep duration predicted accelerated GrimAge in females. These findings suggest that higher substance use presents a mechanism through which earlier maturing youth experience faster epigenetic aging that puts them at risk for poorer health across the lifespan.

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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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