Role of Early Growth Response-1 in the Development of Alcohol-Induced Steatosis

脂肪变性 脂肪肝 肝损伤 肝毒素 酗酒 酒精性肝病 乙醇 纤维化 酒精性脂肪肝 转录因子 生物 内分泌学 肝病 医学 内科学 疾病 生物化学 基因 毒性 肝硬化 精神科
作者
Paul G. Thomes,Terrence M. Donohue
出处
期刊:Current Molecular Pharmacology [Bentham Science Publishers]
卷期号:10 (3): 179-185 被引量:14
标识
DOI:10.2174/1874467208666150817112529
摘要

Here, we describe research on the involvement of the transcription factor, Early Growth Response- 1 (Egr-1) in alcohol-induced liver injury, specifically, fatty liver (steatosis), one of the earliest and most frequent signs of liver injury that occurs after heavy drinking. Egr-1 is a ubiquitous transcription factor found in nearly all cell types. However, because the liver is the principal site of ethanol oxidation, it sustains the greatest damage from alcohol abuse. Thus, this review focuses on how alcohol consumption causes changes in the hepatic expression of Egr-1, which, in turn causes downstream alterations in the expression of other genes to cause liver pathology. Ironically, while such changes in Egr-1 expression clearly favor steatosis and even fibrosis development, the absence of Egr-1 expression can actually exacerbate liver injury after excessive alcohol consumption or after exposure to other hepatotoxins. The existing literature on Egr-1 is extensive. Here, we confine our initial description of Egr-1 to its principal molecular characteristics, its biological functions, and its involvement in certain pathologies that are either directly or obliquely related to alcoholic liver disease. We describe experimental data that clearly implicate Egr-1 function in alcohol-induced steatosis and fibrosis, showing that ethanol-elicited regulation of Egr-1 expression depends on the generation of acetaldehyde and that the absence of Egr-1 diminishes alcohol-induced triglyceride accumulation. Overall, the existing evidence for the involvement of Egr-1 as a key link in alcohol-induced liver disease is strong. The evidence underscores the potential role of Egr-1 and several other transcription factors as therapeutic targets in the alleviation of alcoholic liver disease, which, even after decades of treatment options, still remains difficult to manage in the clinic. Keywords: Egr-1, ethanol, steatosis, lipolysis, autophagy.
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