Pubertal timing as a predictor of epigenetic aging and mortality risk in young adulthood.

IF 3.1 2区心理学 Q2 PSYCHOLOGY, DEVELOPMENTAL Developmental Psychology Pub Date : 2025-01-16 DOI:10.1037/dev0001903

Marlon Goering, Malcolm Barker-Kamps, Amit Patki, Hemant K Tiwari, Sylvie Mrug

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Abstract

Early pubertal timing is associated with adverse health in adulthood. These effects may be mediated by DNA methylation changes associated with accelerated cellular aging and mortality risk, but few studies tested associations between pubertal timing and epigenetic markers in adulthood. Additionally, pubertal timing effects often vary by sex and are understudied in diverse youth. Thus, this longitudinal study examined links between pubertal timing and later epigenetic aging and mortality risk together with sex differences in predominantly Black youth. Participants included 350 individuals (58% female, 42% male; 80% Black, 19% non-Hispanic White). Perceived pubertal timing relative to peers and self-reported phenotypic pubertal timing based on age-adjusted Tanner scores were assessed during early adolescence (M_age = 13) whereas epigenetic aging (GrimAge, DunedinPace of Aging Calculated from the Epigenome, and PhenoAge) and mortality risk were measured during young adulthood (M_age = 27). After adjusting for covariates (smoking, body mass index, family income, early-life stress, race/ethnicity, sex, parenthood), early pubertal timing (both perceived and phenotypic) predicted higher epigenetic mortality risk, and early phenotypic pubertal timing predicted accelerated DunedinPace of Aging Calculated from the Epigenome. Both perceived and phenotypic early pubertal timing were correlated with accelerated GrimAge. Off-time phenotypic pubertal timing (i.e., early and late) was associated with accelerated PhenoAge in males only whereas perceived off-time pubertal timing was unexpectedly linked with lower PhenoAge acceleration. These findings extend prior research by linking two dimensions of early pubertal timing with epigenetic mortality risk and accelerated aging in racially diverse young adults and showing nonlinear effects on PhenoAge acceleration that differ across pubertal timing measures and show some sex differences. (PsycInfo Database Record (c) 2025 APA, all rights reserved).

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青春期时间作为年轻成年期表观遗传衰老和死亡风险的预测因子。

青春期过早与成年后的不良健康状况有关。这些影响可能是由与细胞加速衰老和死亡风险相关的DNA甲基化变化介导的，但很少有研究测试青春期时间与成年期表观遗传标记之间的关系。此外，青春期时间的影响往往因性别而异，在不同的青少年中还没有得到充分的研究。因此，这项纵向研究考察了青春期时间与后来的表观遗传衰老和死亡风险之间的联系，以及主要是黑人青年的性别差异。参与者包括350人(女性58%，男性42%；黑人占80%，非西班牙裔白人占19%)。在青春期早期（Mage = 13）评估相对于同龄人的感知青春期时间和基于年龄调整Tanner评分的自我报告的表型青春期时间，而在青年期（Mage = 27）测量表观遗传衰老（GrimAge，从表观基因组计算的DunedinPace of aging）和死亡风险（Mage = 27）。在调整协变量（吸烟、体重指数、家庭收入、早期生活压力、种族/民族、性别、亲子关系）后，较早的青春期时间（包括感知和表型）预测较高的表观遗传死亡风险，较早的表型青春期时间预测从表观基因组计算的邓尼丁衰老速度加快。感知性和表现性的青春期早期时间均与GrimAge加速相关。在男性中，非正常表型的青春期时间（即早和晚）与加速的表型age有关，而感知到的非正常青春期时间与较低的表型age加速出乎意料地相关。这些发现扩展了先前的研究，将不同种族的年轻人的青春期早期时间与表观遗传死亡风险和加速衰老的两个维度联系起来，并显示出不同青春期时间测量对表型加速的非线性影响，并显示出一些性别差异。（PsycInfo Database Record (c) 2025 APA，版权所有）。

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

Developmental Psychology PSYCHOLOGY, DEVELOPMENTAL-

CiteScore

5.80

自引率

2.50%

发文量

329

期刊介绍： Developmental Psychology ® publishes articles that significantly advance knowledge and theory about development across the life span. The journal focuses on seminal empirical contributions. The journal occasionally publishes exceptionally strong scholarly reviews and theoretical or methodological articles. Studies of any aspect of psychological development are appropriate, as are studies of the biological, social, and cultural factors that affect development. The journal welcomes not only laboratory-based experimental studies but studies employing other rigorous methodologies, such as ethnographies, field research, and secondary analyses of large data sets. We especially seek submissions in new areas of inquiry and submissions that will address contradictory findings or controversies in the field as well as the generalizability of extant findings in new populations. Although most articles in this journal address human development, studies of other species are appropriate if they have important implications for human development. Submissions can consist of single manuscripts, proposed sections, or short reports.