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Chronic ethanol feeding alters miRNA expression dynamics during liver regeneration.

机译:慢性乙醇喂养改变肝脏再生过程中的miRNa表达动态。

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摘要

BACKGROUND: Adaptation to chronic ethanol (EtOH) treatment of rats results in a changed functional state of the liver and greatly inhibits its regenerative ability, which may contribute to the progression of alcoholic liver disease.METHODS: In this study, we investigated the effect of chronic EtOH intake on hepatic microRNA (miRNA) expression in male Sprague-Dawley rats during the initial 24 hours of liver regeneration following 70% partial hepatectomy (PHx) using miRNA microarrays. miRNA expression during adaptation to EtOH was investigated using RT-qPCR. Nuclear factor kappa B (NFκB) binding at target miRNA promoters was investigated with chromatin immunoprecipitation.RESULTS: Unsupervised clustering of miRNA expression profiles suggested that miRNA expression was more affected by chronic EtOH feeding than by the acute challenge of liver regeneration after PHx. Several miRNAs that were significantly altered by chronic EtOH feeding, including miR-34a, miR-103, miR-107, and miR-122 have been reported to play a role in regulating hepatic metabolism and the onset of these miRNA changes occurred gradually during the time course of EtOH feeding. Chronic EtOH feeding also altered the dynamic miRNA profile during liver regeneration. Promoter analysis predicted a role for NFκB in the immediate-early miRNA response to PHx. NFκB binding at target miRNA promoters in the chronic EtOH-fed group was significantly altered and these changes directly correlated with the observed expression dynamics of the target miRNA.CONCLUSIONS: Chronic EtOH consumption alters the hepatic miRNA expression profile such that the response of the metabolism-associated miRNAs occurs during long-term adaptation to EtOH rather than as an acute transient response to EtOH metabolism. Additionally, the dynamic miRNA program during liver regeneration in response to PHx is altered in the chronically EtOH-fed liver and these differences reflect, in part, differences in miRNA expression between the EtOH-adapted and control livers at the baseline state prior to PHx.
机译:背景:适应大鼠慢性乙醇(EtOH)导致肝脏功能状态的改变,并大大抑制其再生能力,这可能有助于酒精性肝病的进展。方法:在这项研究中,我们研究了肝硬化的作用。使用miRNA微阵列技术在70%部分肝切除(PHx)后肝脏再生的最初24小时内,在雄性Sprague-Dawley大鼠中长期摄取EtOH对肝脏microRNA(miRNA)表达的影响。使用RT-qPCR研究了适应EtOH期间的miRNA表达。结果:染色质免疫沉淀研究了核因子κB(NFκB)与靶标miRNA启动子的结合。结果:miRNA表达谱的无监督聚类表明,慢性EtOH喂养对miRNA表达的影响大于PHx后肝脏再生的急性挑战。据报道,一些长期被EtOH喂养而显着改变的miRNA,包括miR-34a,miR-103,miR-107和miR-122,在调节肝脏代谢中起着重要作用,并且这些miRNA的改变在发作期间逐渐发生。 EtOH进料的时间过程。慢性EtOH喂养还改变了肝脏再生过程中的动态miRNA谱。启动子分析预测了NFκB在早期miRNA对PHx的应答中的作用。慢性EtOH喂养组中靶miRNA启动子上的NFκB结合发生了显着改变,这些变化与观察到的靶miRNA表达动力学直接相关。结论:长期摄入EtOH会改变肝miRNA的表达谱,从而代谢-相关的miRNA在长期适应EtOH期间发生,而不是对EtOH代谢的急性短暂反应。此外,在慢性EtOH喂养的肝脏中,响应PHx的肝脏再生过程中动态miRNA程序发生了变化,这些差异部分反映了在pHx之前,处于基线状态的EtOH适应肝脏和对照肝脏之间miRNA表达的差异。

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