早期生命创伤的全基因组表观遗传调控。

Benoit Labonté, Matt Suderman, Gilles Maussion, Luis Navaro, Volodymyr Yerko, Ian Mahar, Alexandre Bureau, Naguib Mechawar, Moshe Szyf, Michael J Meaney, Gustavo Turecki
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引用次数: 456

摘要

背景:我们的基因组适应环境影响,部分是通过表观遗传机制,包括DNA甲基化。啮齿动物早期环境质量的变化与DNA甲基化的改变有关,最近的数据表明,人类对早期生活逆境的反应也有类似的过程。目的:探讨早期创伤引起的全基因组DNA甲基化改变。设计:儿童时期重度虐待个体启动子甲基化的全基因组研究。患者、环境和主要结果测量:41名法裔加拿大男性(25名有严重儿童期虐待史,16名对照组)的海马组织中,使用甲基化DNA免疫沉淀和微阵列杂交技术分析启动子DNA甲基化水平。甲基化谱与信使RNA微阵列获得的相应全基因组基因表达谱进行了比较。通过荧光辅助细胞分选分离的神经元和非神经元DNA片段验证了组间甲基化差异。通过荧光素酶测定评估位点特异性启动子甲基化的功能后果。结果:与对照组相比,我们在有滥用史的个体中发现了362个甲基化差异启动子。在这些启动子中,248个表现出高甲基化,114个表现出低甲基化。5个高度甲基化基因启动子的DNA甲基化验证和位点特异性定量表明,甲基化差异主要发生在神经元细胞部分。参与细胞/神经元可塑性的基因是差异甲基化最显著的基因之一,其中,Alsin (ALS2)是最显著的发现。在虐待自杀完成者的样本中,模拟甲基化状态的甲基化ALS2结构显示,启动子转录活性降低与ALS2变体海马表达降低相关。结论:童年逆境与海马神经元若干基因启动子的表观遗传改变有关。
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Genome-wide epigenetic regulation by early-life trauma.

Context: Our genome adapts to environmental influences, in part through epigenetic mechanisms, including DNA methylation. Variations in the quality of the early environment are associated with alterations in DNA methylation in rodents, and recent data suggest similar processes in humans in response to early-life adversity.

Objective: To determine genome-wide DNA methylation alterations induced by early-life trauma.

Design: Genome-wide study of promoter methylation in individuals with severe abuse during childhood. PATIENTS, SETTING, AND MAIN OUTCOME MEASURES: Promoter DNA methylation levels were profiled using methylated DNA immunoprecipitation followed by microarray hybridization in hippocampal tissue from 41 French-Canadian men (25 with a history of severe childhood abuse and 16 control subjects). Methylation profiles were compared with corresponding genome-wide gene expression profiles obtained by messenger RNA microarrays. Methylation differences between groups were validated on neuronal and nonneuronal DNA fractions isolated by fluorescence-assisted cell sorting. Functional consequences of site-specific promoter methylation were assessed by luciferase assays.

Results: We identified 362 differentially methylated promoters in individuals with a history of abuse compared with controls. Among these promoters, 248 showed hypermethylation and 114 demonstrated hypomethylation. Validation and site-specific quantification of DNA methylation in the 5 most hypermethylated gene promoters indicated that methylation differences occurred mainly in the neuronal cellular fraction. Genes involved in cellular/neuronal plasticity were among the most significantly differentially methylated, and, among these, Alsin (ALS2) was the most significant finding. Methylated ALS2 constructs mimicking the methylation state in samples from abused suicide completers showed decreased promoter transcriptional activity associated with decreased hippocampal expression of ALS2 variants.

Conclusion: Childhood adversity is associated with epigenetic alterations in the promoters of several genes in hippocampal neurons.

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来源期刊
Archives of general psychiatry
Archives of general psychiatry 医学-精神病学
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