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首页> 外文期刊>Epigenetics: official journal of the DNA Methylation Society >Validation of differential GDAP1 DNA methylation in alcohol dependence and its potential function as a biomarker for disease severity and therapy outcome
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Validation of differential GDAP1 DNA methylation in alcohol dependence and its potential function as a biomarker for disease severity and therapy outcome

机译:验证酒精依赖中差异性GDAP1 DNA甲基化及其作为疾病严重程度和治疗结果的生物标志物的潜在功能

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摘要

Alcohol dependence is a severe disorder contributing substantially to the global burden of disease. Despite the detrimental consequences of chronic alcohol abuse and dependence, effective prevention strategies as well as treatment options are largely missing to date. Accumulating evidence suggests that gene-environment interactions, including epigenetic mechanisms, play a role in the etiology of alcohol dependence. A recent epigenome-wide study reported widespread alterations of DNA methylation patterns in alcohol dependent patients compared to control individuals. In the present study, we validate and replicate one of the top findings from this previous investigation in an independent cohort: the hypomethylation of GDAP1 in patients. To our knowledge, this is the first independent replication of an epigenome-wide finding in alcohol dependence. Furthermore, the AUDIT as well as the GSI score were negatively associated with GDAP1 methylation and we found a trend toward a negative association between GDAP1 methylation and the years of alcohol dependency, pointing toward a potential role of GDAP1 hypomethylation as biomarker for disease severity. In addition, we show that the hypomethylation of GDAP1 in patients reverses during a short-term alcohol treatment program, suggesting that GDAP1 DNA methylation could also serve as a potential biomarker for treatment outcome. Our data add to the growing body of knowledge on epigenetic effects in alcohol dependence and support GDAP1 as a novel candidate gene implicated in this disorder. As the role of GDAP1 in alcohol dependence is unknown, this novel candidate gene should be followed up in future studies.
机译:酒精依赖是一种严重的疾病,严重加剧了全球疾病负担。尽管长期滥用酒精和依赖酒精会带来不利影响,但迄今为止,仍缺乏有效的预防策略和治疗选择。越来越多的证据表明,基因与环境的相互作用,包括表观遗传机制,在酒精依赖的病因学中起作用。最近一项有关表观基因组的研究报告说,与对照组相比,酒精依赖患者的DNA甲基化模式发生了广泛变化。在本研究中,我们在独立的队列中验证并复制了先前研究的主要发现之一:患者中GDAP1的甲基化不足。就我们所知,这是酒精依赖中一个表观基因组研究结果的首次独立复制。此外,AUDIT和GSI评分与GDAP1甲基化呈负相关,我们发现GDAP1甲基化与酒精依赖年限之间呈负相关趋势,这表明GDAP1甲基化低下可能是疾病严重程度的生物标志物。此外,我们显示,在短期酒精治疗计划期间,患者中GDAP1的低甲基化现象发生了逆转,这表明GDAP1 DNA甲基化也可以作为治疗结果的潜在生物标志物。我们的数据增加了对酒精依赖的表观遗传学影响的知识,并支持GDAP1作为与这种疾病有关的新候选基因。由于尚不知道GDAP1在酒精依赖中的作用,因此该新的候选基因应在以后的研究中进行随访。

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