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酒精依赖加速表观遗传衰老。

Accelerated epigenetic aging in alcohol dependence.

机构信息

Department of Psychiatry, Kobe University Graduate School of Medicine, Kobe, Japan.

Department of Psychiatry, Kobe University Graduate School of Medicine, Kobe, Japan.

出版信息

J Psychiatr Res. 2024 May;173:175-182. doi: 10.1016/j.jpsychires.2024.03.025. Epub 2024 Mar 23.

Abstract

Alcohol dependence poses a global health threat associated with aging and reduced life expectancy. Recently, aging research through deoxyribonucleic acid (DNA) methylation has gained attention. New epigenetic clocks have been developed; however, no study has investigated GrimAge components, GrimAge2 components and DunedinPACE in patients with alcohol dependence. In this study, we aimed to perform epigenetic clock analysis to evaluate epigenetic age acceleration and DNA methylation-based age-predictive components in patients with alcohol dependence and controls. We utilized publicly available DNA methylation data (GSE98876) for our analysis. Additionally, we compared the values of the same items before and after the patients underwent a treatment program. The dataset comprised 23 controls and 24 patients. We observed that DunedinPACE accelerated more in patients with alcohol dependence. AgeAccelGrim and AgeAccelGrim2 decelerated more after the treatment program than before, and beta-2-microglobulin and Cystatin C decreased after the treatment program than before. These findings are crucial as they affect the cranial nerve area, potentially contributing to cognitive dysfunction and psychiatric symptoms in patients with alcohol dependence.

摘要

酒精依赖是一种全球性的健康威胁,与衰老和预期寿命缩短有关。最近,通过脱氧核糖核酸(DNA)甲基化进行衰老研究引起了关注。已经开发出了新的表观遗传时钟,但没有研究调查过酒精依赖患者的 GrimAge 成分、GrimAge2 成分和 DunedinPACE。在这项研究中,我们旨在进行表观遗传时钟分析,以评估酒精依赖患者和对照组的表观遗传年龄加速和基于 DNA 甲基化的年龄预测成分。我们利用了公开的 DNA 甲基化数据(GSE98876)进行分析。此外,我们还比较了患者接受治疗前后相同项目的值。该数据集包括 23 名对照者和 24 名患者。我们观察到酒精依赖患者的 DunedinPACE 加速更多。治疗后,AgeAccelGrim 和 AgeAccelGrim2 的减速比治疗前更明显,β-2-微球蛋白和胱抑素 C 在治疗后比治疗前减少。这些发现很重要,因为它们会影响颅神经区域,可能导致酒精依赖患者认知功能障碍和精神症状。

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