首页> 外文期刊>Journal of Hepatology: The Journal of the European Association for the Study of the Liver >The impact of CYP2E1 on the development of alcoholic liver disease as studied in a transgenic mouse model.
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The impact of CYP2E1 on the development of alcoholic liver disease as studied in a transgenic mouse model.

机译:CYP2E1对酒精性肝病发展的影响,在转基因小鼠模型中进行了研究。

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BACKGROUND/AIMS: CYP2E1 metabolizes ethanol, generates reactive oxygen species, and is suggested to be important for development of alcoholic liver disease. The present study aims to evaluate the role of CYP2E1 in combination with ethanol for development of alcoholic liver disease using mice transgenic for the human CYP2E1 gene. METHODS: Changes in hepatic gene expression were monitored in controls and mice transgenic for human CYP2E1, treated with ethanol or isocaloric dextrose intragastrically for 4 weeks, and related to pathology using Affymetrix microarrays and TaqMan RealTime PCR. RESULTS: Presence of the CYP2E1 transgene increased liver injury and increased expression of stress related genes. Microarray analyses revealed the expression of structural genes, particularly cytokeratin 8 and 18, to be highly related to pathology. CONCLUSIONS: This in vivo study confirms several findings regarding CYP2E1 and alcohol previously found only in vitro. These results provide in vivo evidence that CYP2E1 overexpression aggravates hepatic injury, and suggest that expression of cytokeratins 8 and 18 can be considered as biomakers for the progression of alcoholic liver disease.
机译:背景/目的:CYP2E1代谢乙醇,产生活性氧,被认为对酒精性肝病的发展很重要。本研究旨在评估CYP2E1与乙醇联合使用对人CYP2E1基因转基因的小鼠在酒精性肝病发展中的作用。方法:在对照组和转基因人类CYP2E1小鼠中监测肝基因表达的变化,用乙醇或等渗葡萄糖在胃内处理4周,并使用Affymetrix微阵列和TaqMan RealTime PCR与病理学相关。结果:CYP2E1转基因的存在增加了肝损伤和应激相关基因的表达增加。微阵列分析显示结构基因的表达,特别是细胞角蛋白8和18与病理高度相关。结论:该体内研究证实了先前仅在体外发现的有关CYP2E1和酒精的一些发现。这些结果提供了体内证据,表明CYP2E1过表达加重了肝损伤,并提示细胞角蛋白8和18的表达可被认为是酒精性肝病发展的生物制造者。

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