铁调节激素铁调素是酒精性肝病的危险因素吗?
Is the iron regulatory hormone hepcidin a risk factor for alcoholic liver disease?
作者信息
Harrison-Findik Duygu Dee
机构信息
Division of Gastroenterology and Hepatology, Department of Internal Medicine, University of Nebraska Medical Center, Omaha, NE, 68198-5820, United States.
出版信息
World J Gastroenterol. 2009 Mar 14;15(10):1186-93. doi: 10.3748/wjg.15.1186.
Despite heavy consumption over a long period of time, only a small number of alcoholics develop alcoholic liver disease. This alludes to the possibility that other factors, besides alcohol, may be involved in the progression of the disease. Over the years, many such factors have indeed been identified, including iron. Despite being crucial for various important biological processes, iron can also be harmful due to its ability to catalyze Fenton chemistry. Alcohol and iron have been shown to interact synergistically to cause liver injury. Iron-mediated cell signaling has been reported to be involved in the pathogenesis of experimental alcoholic liver disease. Hepcidin is an iron-regulatory hormone synthesized by the liver, which plays a pivotal role in iron homeostasis. Both acute and chronic alcohol exposure suppress hepcidin expression in the liver. The sera of patients with alcoholic liver disease, particularly those exhibiting higher serum iron indices, have also been reported to display reduced prohepcidin levels. Alcohol-mediated oxidative stress is involved in the inhibition of hepcidin promoter activity and transcription in the liver. This in turn leads to an increase in intestinal iron transport and liver iron storage. Hepcidin is expressed primarily in hepatocytes. It is noteworthy that both hepatocytes and Kupffer cells are involved in the progression of alcoholic liver disease. However, the activation of Kupffer cells and TNF-alpha signaling has been reported not to be involved in the down-regulation of hepcidin expression by alcohol in the liver. Alcohol acts within the parenchymal cells of the liver to suppress the synthesis of hepcidin. Due to its crucial role in the regulation of body iron stores, hepcidin may act as a secondary risk factor in the progression of alcoholic liver disease. The clarification of the mechanisms by which alcohol disrupts iron homeostasis will allow for further understanding of the pathogenesis of alcoholic liver disease.
尽管长期大量饮酒,但只有少数酗酒者会发展为酒精性肝病。这暗示了除酒精外,其他因素可能也参与了该疾病的进展。多年来,确实已经发现了许多这样的因素,包括铁。尽管铁对各种重要的生物过程至关重要,但由于其催化芬顿化学反应的能力,它也可能是有害的。酒精和铁已被证明具有协同作用,可导致肝损伤。据报道铁介导的细胞信号传导参与实验性酒精性肝病的发病机制。铁调素是一种由肝脏合成的铁调节激素,在铁稳态中起关键作用。急性和慢性酒精暴露均会抑制肝脏中铁调素的表达。据报道,酒精性肝病患者的血清,尤其是那些血清铁指标较高的患者,其血清中铁调素原水平也会降低。酒精介导的氧化应激参与了肝脏中铁调素启动子活性和转录的抑制。这进而导致肠道铁转运增加和肝脏铁储存增加。铁调素主要在肝细胞中表达。值得注意的是,肝细胞和库普弗细胞均参与酒精性肝病的进展。然而,据报道库普弗细胞的激活和肿瘤坏死因子-α信号传导不参与酒精对肝脏中铁调素表达的下调。酒精在肝脏实质细胞内起作用,抑制铁调素的合成。由于其在调节体内铁储存方面的关键作用,铁调素可能在酒精性肝病的进展中作为次要危险因素。阐明酒精破坏铁稳态的机制将有助于进一步了解酒精性肝病的发病机制。
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