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Immediate-early alcohol-responsive miRNA expression in Drosophila

机译:在果蝇中立即早期的酒精响应性miRNA表达

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At the core of the changes characteristic of alcoholism are alterations in gene expression in the brain of the addicted individual. These changes are believed to underlie some of the neuroadaptations that promote compulsive drinking. Unfortunately, the mechanisms by which alcohol consumption produces changes in gene expression remain poorly understood. MicroRNAs (miRNAs) have emerged as important regulators of gene expression because they can coordinately modulate the translation efficiency of large sets of specific mRNAs. Here, we investigate the early miRNA responses elicited by an acute sedating dose of alcohol in the Drosophila model organism. In our analysis, we combine the power of next-generation sequencing with Drosophila genetics to identify alcohol-sensitive miRNAs and to functionally test them for a role in modulating alcohol sensitivity. We identified 14 known Drosophila miRNAs, and 13 putative novel miRNAs that respond to an acute sedative exposure to alcohol. Using the GeneSwitch Gal4/UAS system, a subset of these ethanol-responsive miRNAs was functionally tested to determine their individual contribution in modulating ethanol sensitivity. We identified two microRNAs that when overexpressed significantly increased ethanol sensitivity: miR-6 and miR-310. MicroRNA target prediction analysis revealed that the different alcohol-responsive miRNAs target-overlapping sets of mRNAs. Alcoholism is the product of accumulated cellular changes produced by chronic ethanol consumption. Although all of the changes described herein are extremely rapid responses evoked by a single ethanol exposure, understanding the gene expression changes that occur in the first few minutes after ethanol exposure will help us to categorize ethanol responses into those that are near instantaneous and those that are emergent responses produced only by repeated ethanol exposure.
机译:在酗酒的变化的核心,是上瘾的人的大脑中基因表达的改变。这些变化被认为是促进强迫饮酒的一些神经面具。不幸的是,醇消耗产生基因表达变化的机制仍然明显不知。 MicroRNAS(miRNA)已成为基因表达的重要调节因子,因为它们可以协调大套特定MRNA的翻译效率。在这里,我们研究了在果蝇模型生物中急性镇静剂量的醇引发的早期miRNA反应。在我们的分析中,我们将下一代测序与果蝇遗传学的力量结合起来鉴定酒精敏感的miRNA,并在调节醇敏感性方面的作用进行功能测试。我们鉴定了14名已知的果蝇MiRNA,13名推定新的miRNA,可应对急性镇静暴露于酒精。使用GenesWitch Gal4 / UAS系统,在功能上测试这些乙醇响应性miRNA的子集,以确定它们在调节乙醇敏感性方面的个体贡献。我们鉴定了两种微小RNA,当过表达显着增加的乙醇敏感性:miR-6和miR-310。 MicroRNA靶预测分析显示,不同的醇响应MiRNA靶重叠的MRNA。酗酒是通过慢性乙醇消耗产生的累积细胞变化的产物。虽然本文所述的所有变化是由单次乙醇暴露引起的极快反应,但了解乙醇暴露后的最初几分钟内发生的基因表达变化,这将有助于我们将乙醇反应分类为近瞬间的乙醇反应和那些仅通过反复乙醇暴露产生的紧急反应。

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