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综述:DNA甲基化与酒精使用障碍:进展与挑战

Review: DNA methylation and alcohol use disorders: Progress and challenges.

作者信息

Zhang Huiping, Gelernter Joel

机构信息

Department of Psychiatry, Yale University School of Medicine, New Haven, Connecticut.

VA Connecticut Healthcare System, West Haven, Connecticut.

出版信息

Am J Addict. 2017 Aug;26(5):502-515. doi: 10.1111/ajad.12465. Epub 2016 Oct 19.

Abstract

BACKGROUND AND OBJECTIVES

Risk for alcohol use disorders (AUDs) is influenced by gene-environment interactions. Environmental factors can affect gene expression through epigenetic mechanisms such as DNA methylation. This review outlines the findings regarding the association of DNA methylation and AUDs.

METHODS

We searched PubMed (by April 2016) and identified 29 studies that examined the association of DNA methylation and AUDs. We also evaluated the methods used in these studies.

RESULTS

Two studies demonstrated elevated global (repetitive element) DNA methylation levels in AUD subjects. Fifteen candidate gene studies showed hypermethylation of promoter regions of six genes (AVP, DNMT3B, HERP, HTR3A, OPRM1, and SNCA) or hypomethylation of the GDAP1 promoter region in AUD subjects. Five genome-wide DNA methylation studies demonstrated widespread DNA methylation changes across the genome in AUD subjects. Six studies showed significant correlations of DNA methylation with gene expression in AUD subjects. Three studies revealed interactive effects of genetic variation and DNA methylation on susceptibility to AUDs. Most studies analyzed AUD-associated DNA methylation changes in the peripheral blood; a few studies examined DNA methylation changes in postmortem brains of AUD subjects.

DISCUSSION AND CONCLUSIONS

Chronic alcohol consumption may result in DNA methylation changes, leading to neuroadaptations that may underlie some of the mechanisms of AUD risk and persistence. Future studies are needed to confirm the few existing results, and then to elucidate whether DNA methylation changes are the cause or consequence of AUDs.

SCIENTIFIC SIGNIFICANCE

DNA methylation profiles may be used to assess AUD status or monitor AUD treatment response. (Am J Addict 2017;26:502-515).

摘要

背景与目的

酒精使用障碍(AUDs)的风险受基因-环境相互作用的影响。环境因素可通过DNA甲基化等表观遗传机制影响基因表达。本综述概述了有关DNA甲基化与AUDs关联的研究结果。

方法

我们检索了PubMed(截至2016年4月),确定了29项研究DNA甲基化与AUDs关联的研究。我们还评估了这些研究中使用的方法。

结果

两项研究表明AUD患者的整体(重复元件)DNA甲基化水平升高。15项候选基因研究显示,AUD患者中6个基因(AVP、DNMT3B、HERP、HTR3A、OPRM1和SNCA)的启动子区域存在高甲基化,或GDAP1启动子区域存在低甲基化。5项全基因组DNA甲基化研究表明,AUD患者的全基因组存在广泛的DNA甲基化变化。6项研究表明,AUD患者中DNA甲基化与基因表达存在显著相关性。3项研究揭示了基因变异和DNA甲基化对AUD易感性的交互作用。大多数研究分析了外周血中与AUD相关的DNA甲基化变化;少数研究检测了AUD患者死后大脑中的DNA甲基化变化。

讨论与结论

长期饮酒可能导致DNA甲基化变化,从而引起神经适应性改变,这可能是AUD风险和持续性某些机制的基础。未来需要进行研究以证实现有的少量结果,进而阐明DNA甲基化变化是AUD的原因还是结果。

科学意义

DNA甲基化谱可用于评估AUD状态或监测AUD治疗反应。(《美国成瘾杂志》2017年;26:502 - 515)

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