英国儿童的不良童年经历、DNA 甲基化年龄加速与皮质醇:一项基于人群的前瞻性队列研究。
Adverse childhood experiences, DNA methylation age acceleration, and cortisol in UK children: a prospective population-based cohort study.
机构信息
Bristol Medical School, Faculty of Health Sciences, University of Bristol, 5 Tyndall Avenue, Bristol, BS8 1UD, UK.
Keenan Research Centre for Biomedical Science, St. Michael's Hospital, Toronto, Canada.
出版信息
Clin Epigenetics. 2020 Apr 7;12(1):55. doi: 10.1186/s13148-020-00844-2.
BACKGROUND
Epigenetic mechanisms may partly explain the persistent effects of adverse childhood experiences (ACEs) on health outcomes in later life. DNA methylation can predict chronological age, and advanced methylation-predicted age beyond chronological age (DNA methylation age acceleration) is associated with ACEs, adverse mental and physical health, and elevated diurnal and baseline salivary cortisol. Childhood adversity is also associated with dysregulation of the hypothalamic-pituitary-adrenal axis, which produces the neuroendocrine hormone cortisol. It remains unknown whether these associations are specific to certain types of adversity. Herein, we investigate the associations of ACEs with DNA methylation age acceleration and plasma cortisol in the Avon Longitudinal Study of Parents and Children (ALSPAC) birth cohort.
METHODS
In this study of the children in ALSPAC, we used multiple linear regression to examine associations of cumulative exposure to ACE, as well as exposure to ten individual types of ACEs, with Horvath-estimated DNA methylation age acceleration and with baseline plasma cortisol. The ten ACEs were those included in the World Health Organization's ACE International Questionnaire. Data on ACEs were prospectively collected from age 0-14 years. DNA methylation age acceleration and plasma cortisol were measured at mean 17.1 years and 15.5 years, respectively.
RESULTS
We included 974 UK children in the present study. Exposure to four or more ACEs compared to zero was associated with DNA methylation age acceleration in girls (β, 95% CI = 1.65, 0.25 to 3.04 years) but not in boys (β, 95% CI = - 0.11, - 1.48 to 1.26 years). Also, in girls, emotional abuse and physical abuse were each associated with DNA methylation age acceleration (β, 95% CI = 1.20, 0.15 to 2.26 years and β, 95% CI = 1.22, 0.06 to 2.38 years, respectively). No other ACEs were associated with accelerated DNA methylation age in either sex. Associations were also null between ACE and cortisol, and cortisol and DNA methylation age acceleration.
CONCLUSIONS
In this prospective population-based study of UK children, cumulative ACE exposure, emotional abuse, and physical abuse between age 0 and 14 years were each associated with Horvath-estimated DNA methylation age acceleration at age 17 years in girls but not in boys.
背景
表观遗传机制可能部分解释了童年逆境(ACEs)对晚年健康结果的持久影响。DNA 甲基化可以预测实际年龄,而预测年龄超过实际年龄的先进甲基化(DNA 甲基化年龄加速)与 ACEs、不良的精神和身体健康以及昼夜和基线唾液皮质醇升高有关。童年逆境也与下丘脑-垂体-肾上腺轴的失调有关,该轴产生神经内分泌激素皮质醇。目前尚不清楚这些关联是否特定于某些类型的逆境。在此,我们在阿冯纵向研究父母和儿童(ALSPAC)出生队列中调查了 ACEs 与 DNA 甲基化年龄加速和血浆皮质醇的关系。
方法
在这项针对 ALSPAC 儿童的研究中,我们使用多元线性回归来检验累积 ACE 暴露以及暴露于十种特定 ACE 类型与 Horvath 估计的 DNA 甲基化年龄加速和基线血浆皮质醇之间的关系。十种 ACE 是世界卫生组织 ACE 国际问卷中包含的 ACE。ACE 数据从 0-14 岁前瞻性收集。DNA 甲基化年龄加速和血浆皮质醇分别在平均 17.1 岁和 15.5 岁测量。
结果
我们纳入了 974 名英国儿童进行本研究。与零 ACEs 相比,暴露于四种或更多 ACEs 与女孩的 DNA 甲基化年龄加速相关(β,95%CI=1.65,0.25 至 3.04 岁),但与男孩无关(β,95%CI=-0.11,-1.48 至 1.26 岁)。此外,在女孩中,情感虐待和身体虐待均与 DNA 甲基化年龄加速相关(β,95%CI=1.20,0.15 至 2.26 岁和β,95%CI=1.22,0.06 至 2.38 岁)。在任何性别中,其他 ACEs 均与加速的 DNA 甲基化年龄无关。ACE 与皮质醇之间以及皮质醇与 DNA 甲基化年龄加速之间的关联也为零。
结论
在这项针对英国儿童的前瞻性基于人群的研究中,0-14 岁期间的累积 ACE 暴露、情感虐待和身体虐待与女孩 17 岁时的 Horvath 估计 DNA 甲基化年龄加速有关,但与男孩无关。
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