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出生时的表观遗传时钟:与母亲产前抑郁和儿童精神问题的关联。

The Epigenetic Clock at Birth: Associations With Maternal Antenatal Depression and Child Psychiatric Problems.

机构信息

University of Helsinki, Finland.

Max-Planck Institute of Psychiatry, Germany.

出版信息

J Am Acad Child Adolesc Psychiatry. 2018 May;57(5):321-328.e2. doi: 10.1016/j.jaac.2018.02.011. Epub 2018 Mar 15.

Abstract

OBJECTIVE

Maternal antenatal depression may compromise the fetal developmental milieu and contribute to individual differences in aging and disease trajectories in later life. We evaluated the association between maternal antenatal depression and a novel biomarker of aging at birth, namely epigenetic gestational age (GA) based on fetal cord blood methylation data. We also examined whether this biomarker prospectively predicts and mediates maternal effects on early childhood psychiatric problems.

METHOD

A total of 694 mothers from the Prediction and Prevention of Preeclampsia and Intrauterine Growth Restriction (PREDO) Study provided information on history of depression diagnosed before pregnancy; 581 completed the Center for Epidemiological Studies Depression Scale throughout pregnancy, and 407 completed the Child Behavior Checklist at child's age 3.7 years (SD = 0.75 year). DNA methylation (DNAm) GA of fetal cord blood DNA was based on the methylation profile of 148 selected cytosine linked to guanine by phosphate (CpG) sites. Epigenetic GA was calculated as the arithmetic difference between DNAm GA and chronological GA and adjusted for chronological GA.

RESULTS

Maternal history of depression diagnosed before pregnancy (mean difference = -0.25 SD units, 95% CI = -0.46 to -0.03) and greater antenatal depressive symptoms (-0.08 SD unit per 1-SD unit increase, 95% CI = -0.16 to -0.004) were associated with child's lower epigenetic GA. Child's lower epigenetic GA, in turn, prospectively predicted total and internalizing problems and partially mediated the effects of maternal antenatal depression on internalizing problems in boys.

CONCLUSION

Maternal antenatal depression is associated with lower epigenetic GA in offspring. This lower epigenetic GA seems to be associated with a developmental disadvantage for boys, who, in early childhood, show greater psychiatric problems.

摘要

目的

孕妇产前抑郁可能会损害胎儿发育环境,并导致个体在晚年的衰老和疾病轨迹上存在差异。我们评估了孕妇产前抑郁与一种新的出生时衰老生物标志物(即基于胎儿脐带血甲基化数据的表观遗传孕龄(GA))之间的关联。我们还研究了该生物标志物是否能够前瞻性地预测并调节母亲对幼儿期精神问题的影响。

方法

共有 694 名来自预测和预防子痫前期和宫内生长受限(PREDO)研究的母亲提供了她们在怀孕前被诊断出患有抑郁症的病史信息;其中 581 名母亲在整个怀孕期间完成了流行病学研究中心抑郁量表,407 名母亲在孩子 3.7 岁(SD=0.75 岁)时完成了儿童行为检查表。胎儿脐带血 DNA 的 DNAmGA 是基于与磷酸相连的 148 个选定的胞嘧啶鸟嘌呤(CpG)位点的甲基化谱计算得出的。表观遗传 GA 是通过将 DNAmGA 与实际 GA 的算术差计算得出的,并根据实际 GA 进行了调整。

结果

孕妇产前被诊断出的抑郁症病史(平均差异=-0.25 个 SD 单位,95%CI=-0.46 至-0.03)和更大的产前抑郁症状(每增加 1 个 SD 单位,减少 0.08 个 SD 单位,95%CI=-0.16 至-0.004)与孩子较低的表观遗传 GA 相关。孩子较低的表观遗传 GA 反过来又可以预测总问题和内化问题,并部分调节母亲产前抑郁对男孩内化问题的影响。

结论

孕妇产前抑郁与后代的低表观遗传 GA 相关。这种较低的表观遗传 GA 似乎与男孩的发育劣势有关,他们在幼儿期表现出更大的精神问题。

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