首页> 外文期刊>Alcoholism: Clinical and experimental research >Convergent Evidence From Humans and Drosophila melanogaster Drosophila melanogaster Implicates the Transcription Factor MEF2B MEF2B / Mef2 Mef2 in Alcohol Sensitivity
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Convergent Evidence From Humans and Drosophila melanogaster Drosophila melanogaster Implicates the Transcription Factor MEF2B MEF2B / Mef2 Mef2 in Alcohol Sensitivity

机译:来自人类和果蝇的收敛证据德罗洛拉美洛拉斯司机将转录因子MEF2B MEF2B / MEF2 MEF2含有酒精敏感性

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Background Self‐Rating of the Effects of Alcohol (SRE) measures level of response to ethanol (EtOH) in humans. Interestingly, there is a positive relationship between the SRE and risk for abusing alcohol, suggesting mechanistic connections between SRE and alcohol abuse. Methods To identify candidate genes with a role in SRE and alcohol‐related behavior more generally, we coupled human genetic analyses with studies in Drosophila melanogaster . We first performed a gene‐based analysis of Genomewide association studies (GWAS) summary statistics for SRE in the Avon Longitudinal Study of Parents and Children sample. Based on prior findings in humans, orthology to fly genes, and the availability of genetic reagents, we selected a subset of these genes for studies on EtOH behavior in Drosophila . Results We found 37 genes with nominal associations in our SRE GWAS. We explored the role of 6 orthologous genes in Drosophila EtOH sedation and rapid tolerance. We found that the transcription factor Mef2 is required for normal EtOH sedation in flies. Pan‐neuronal expression of 2 independent Mef2 RNAi transgenes significantly reduced Mef2 expression and made flies resistant to EtOH sedation. Additionally, flies with multiple independent mutant alleles of Mef2 were also resistant to EtOH sedation, confirming a role for Mef2 in this behavior. Altered expression of Mef2 did not change EtOH rapid tolerance or cause a net change in internal EtOH concentrations. Conclusions Our studies indicate that MEF2B influences SRE in humans and that Mef2 impacts EtOH sedation in Drosophila .
机译:背景醇(SRE)测量对人体乙醇(EtOH)的反应水平的自我评级。有趣的是,SRE与滥用酒精的风险之间存在积极的关系,暗示SRE和酒精滥用之间的机械联系。方法以鉴定候选基因的作用和与醇相关的行为中的作用更普遍,我们偶联了在果蝇黑素体中的研究人体遗传分析。我们首先进行了基于基于基于基于基于基于基于基于基于基于基于GenoMewide的基因组合研究(GWAS)综述父母和儿童样本的纵向纵向研究的SRE。基于人类的先前发现,矫正基因和遗传试剂的可用性,我们选择了这些基因的子集,用于研究果蝇的EtOH行为。结果我们在我们的SRE GWA中发现了37个基因。我们探讨了6种外科基因在果蝇EtoH镇静和快速耐受的作用。我们发现苍蝇中正常EtOH镇静需要转录因子MEF2。 2个独立MEF2 RNAi转基因的PAN-神经元表达显着降低了MEF2表达,并使耐氧镇静的恒定。另外,具有多种独立突变等位基因的MEF2的苍蝇也抵抗EtOH镇静,证实了MEF2在这种行为中的作用。 MEF2的改变表达未改变EtOH快速耐受,或导致内部EtOH浓度的净变化。结论我们的研究表明MEF2B对人类的影响,并且MEF2在果蝇中影响EtOH镇静。

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