压力性生活事件与年轻人的生物年龄随时间加速老化。
Stressful life events and accelerated biological aging over time in youths.
机构信息
Department of Psychology, University of California, Los Angeles, Psychology Building 1285, Box 951563, Los Angeles, CA 90095, USA.
Department of Occupational and Environmental Health Sciences, Peking University, Xueyuan Rd. 38, Haidian District, Beijing, China; Department of Environmental Health Sciences, Columbia Mailman School of Public Health, 722 W. 168th Street, New York, NY 10032, USA.
出版信息
Psychoneuroendocrinology. 2023 May;151:106058. doi: 10.1016/j.psyneuen.2023.106058. Epub 2023 Feb 17.
Experiencing adversity in childhood and adolescence, including stressful life events (SLEs), may accelerate the pace of development, leading to adverse mental and physical health. However, most research on adverse early experiences and biological aging (BA) in youths relies on cross-sectional designs. In 171 youths followed for approximately 2 years, we examined if SLEs over follow-up predicted rate of change in two BA metrics: epigenetic age and Tanner stage. We also investigated if rate of change in BA was associated with changes in depressive symptoms over time. Youths aged 8-16 years at baseline self-reported Tanner stage and depressive symptoms at baseline and follow-up and provided saliva samples for DNA at both assessments. Horvath epigenetic age estimates were derived from DNA methylation data measured with the Illumina EPIC array. At follow-up, contextual threat interviews were administered to youths and caregivers to assess youths' experiences of past-year SLEs. Interviews were objectively coded by an independent rating team to generate a SLE impact score, reflecting the severity of all SLEs occurring over the prior year. Rate of change in BA metrics was operationalized as change in epigenetic age or Tanner stage as a function of time between assessments. Higher objective SLE impact scores over follow-up were related to a greater rate of change in epigenetic age (β = 0.21, p = .043). Additionally, among youths with lower-but not higher-Tanner stage at baseline, there was a positive association of SLE impact scores with rate of change in Tanner stage (Baseline Tanner Stage × SLE Impact Score interaction: β = - 0.21, p = .011). A greater rate of change in epigenetic age was also associated with higher depressive symptom levels at follow-up, adjusting for baseline symptoms (β = 0.15, p = .043). Associations with epigenetic age were similar, although slightly attenuated, when adjusting for epithelial (buccal) cell proportions. Whereas much research in youths has focused on severe experiences of early adversity, we demonstrate that more commonly experienced SLEs during adolescence may also contribute to accelerated BA. Further research is needed to understand the long-term consequences of changes in BA metrics for health.
在儿童和青少年时期经历逆境,包括生活压力事件 (SLEs),可能会加速发展进程,导致心理健康和身体健康状况不佳。然而,大多数关于青少年不良早期经历和生物衰老 (BA) 的研究都依赖于横断面设计。在大约 2 年的时间里,我们对 171 名青少年进行了跟踪调查,研究了随访期间 SLE 是否预测了两种 BA 指标的变化速度:表观遗传年龄和坦纳阶段。我们还研究了 BA 变化速度是否与随时间推移抑郁症状的变化有关。在基线时,年龄在 8 至 16 岁的青少年自我报告了坦纳阶段和抑郁症状,并在基线和随访时提供了唾液样本进行 DNA 检测。Horvath 表观遗传年龄估计值是从使用 Illumina EPIC 阵列测量的 DNA 甲基化数据中得出的。在随访时,对青少年和照顾者进行了霍维茨环境威胁访谈,以评估青少年过去一年的 SLE 经历。访谈由一个独立的评分小组进行客观编码,以生成 SLE 影响评分,反映过去一年中所有 SLE 的严重程度。BA 指标的变化速度被定义为评估之间时间的表观遗传年龄或坦纳阶段的变化。随访期间更高的客观 SLE 影响评分与表观遗传年龄变化速度更快相关 (β=0.21,p=0.043)。此外,在基线时坦纳阶段较低但不高的青少年中,SLE 影响评分与坦纳阶段变化速度之间存在正相关 (基线坦纳阶段×SLE 影响评分交互作用:β= - 0.21,p=0.011)。调整基线症状后,表观遗传年龄变化速度更快与随访时更高的抑郁症状水平相关 (β=0.15,p=0.043)。当调整上皮 (颊) 细胞比例时,与表观遗传年龄的关联相似,只是略有减弱。虽然青少年时期的早期逆境经历备受关注,但我们的研究表明,青春期更为常见的 SLE 也可能导致 BA 加速。需要进一步研究以了解 BA 指标变化对健康的长期影响。
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