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在一个种族/民族多样化的样本中,表观遗传衰老的多基因风险与不良生活经历相互作用,以预测青少年抑郁症的发展。

Polygenic risk for epigenetic aging and adverse life experiences interact to predict growth in adolescent depression in a racially/ethnically diverse sample.

作者信息

Elam Kit K, Su Jinni, Qin Weisiyu Abraham, Lemery-Chalfant Kathryn

机构信息

Department of Applied Health Science, School of Public Health, Indiana University, Bloomington, IN, United States.

Psychology Department, Arizona State University, Tempe, AZ, United States.

出版信息

Front Psychiatry. 2024 Dec 20;15:1499395. doi: 10.3389/fpsyt.2024.1499395. eCollection 2024.

Abstract

INTRODUCTION

Research has yet to examine the interplay between indices of environmental risk and resilience processes and genetic predisposition for epigenetic aging in predicting early adolescent depressive symptoms. In the current study we examine whether adverse life events and parental acceptance moderate polygenic predisposition for GrimAge epigenetic aging in predicting trajectories of depressive symptoms across early adolescence.

METHOD

Using data from the Adolescent Brain Development Study (ABCD, N = 11,875), we created polygenic scores for GrimAge, and examined whether exposure to adverse life events and parental acceptance moderated the relation between genetic risk and depressive symptom trajectories from age 10/11 to 12/13 using growth mixture modelling. We examined models separately in European American (EA), African American (AA), and Latinx (LX) subgroups of ABCD.

RESULTS

In the EA and AA subgroups, adverse life events moderated polygenic scores for GrimAge such that there was increased likelihood of membership in a higher vs. lower depression trajectory.

DISCUSSION

We extend literature by identifying genetic contributions to epigenetic aging as a depression diathesis in adolescence. Findings also highlight the detrimental role of adverse life events in exacerbating genetic risk for the development of depression in adolescence.

摘要

引言

关于环境风险指数、复原力过程与表观遗传衰老的遗传易感性之间的相互作用在预测青少年早期抑郁症状方面的研究尚少。在本研究中,我们探讨了不良生活事件和父母接纳在预测整个青少年早期抑郁症状轨迹时,是否会调节GrimAge表观遗传衰老的多基因易感性。

方法

利用青少年大脑发育研究(ABCD,N = 11875)的数据,我们创建了GrimAge的多基因评分,并使用生长混合模型研究了暴露于不良生活事件和父母接纳是否会调节10/11岁至12/13岁期间遗传风险与抑郁症状轨迹之间的关系。我们在ABCD的欧美裔(EA)、非裔美国人(AA)和拉丁裔(LX)亚组中分别检验了模型。

结果

在EA和AA亚组中,不良生活事件调节了GrimAge的多基因评分,使得个体进入高抑郁轨迹而非低抑郁轨迹的可能性增加。

讨论

我们通过确定遗传因素对表观遗传衰老的影响是青少年抑郁症素质,扩展了相关文献。研究结果还强调了不良生活事件在加剧青少年抑郁症发生的遗传风险方面的有害作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a8d1/11695374/b7a820eac86a/fpsyt-15-1499395-g001.jpg

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