白蛋白和I型前胶原蛋白基因在酒精和病毒诱导的人肝病中的调控。

G Annoni, B Arosio, D Santambrogio, N Gagliano, M A Zern
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摘要

慢性酒精性肝病的共同特征是进行性低白蛋白血症和肝纤维化。造成这些影响的分子机制仍然存在争议。因此,在本研究中,我们评估了酒精滥用者和病毒性肝病患者肝脏中白蛋白和胶原蛋白基因的表达。在30例接受诊断性肝活检的患者中测定白蛋白和前α 1 (I)胶原mRNA水平。14例饮酒者中,7例单纯为酒精性肝炎,7例肝硬化合并酒精性肝炎。16例非酒精性慢性病毒感染患者中,6例合并慢性活动性肝炎,10例合并肝硬化合并慢性活动性肝炎。从每个活检组织的一部分中提取总RNA,与人白蛋白或胶原cDNA克隆杂交,并与2个正常手术标本作为对照进行比较。Northern杂交研究显示:尽管存在炎症和纤维化,但酗酒者的白蛋白mRNA水平与正常对照相似;这些酗酒者的白蛋白mRNA水平明显高于病毒感染引起的疾病组织学分期相似的患者;与对照组相比,所有类别的患者前胶原mRNA水平均显著升高。鉴于这些结果,我们很容易推测酒精实际上可能会增加人体内白蛋白mRNA的含量,就像它在动物体内一样。此外,纤维化肝脏中前胶原mRNA水平的升高表明胶原合成的增加可能是肝纤维化发病的一个重要因素。
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Albumin and procollagen type I gene regulation in alcohol and viral-induced human liver disease.

Common features of chronic alcoholic liver disease are progressive hypoalbuminemia and liver fibrosis. The molecular mechanisms which account for these effects are still controversial. Therefore, in the present study we evaluated albumin and collagen gene expression in livers of alcohol abusers and patients with viral-induced liver disease. Albumin and pro-alpha 1 (I) collagen mRNA levels were determined in 30 patients who underwent diagnostic liver biopsy. Of 14 alcoholics, 7 had alcoholic hepatitis alone, while the other 7 had cirrhosis plus alcoholic hepatitis. Of 16 non-alcoholic patients with chronic viral infection, 6 had chronic active hepatitis and 10 cirrhosis plus chronic active hepatitis. Total RNA was extracted from a portion of each biopsy, hybridized with a human albumin or collagen cDNA clone and compared to 2 normal surgical specimens which served as controls. The Northern hybridization studies revealed that: despite the presence of inflammation and fibrosis, the albumin mRNA levels of alcoholics were similar to normal controls; these alcoholics had significantly higher levels of albumin mRNA than did patients with similar histological stages of disease due to viral infection; and all the categories of patients had markedly increased procollagen mRNA levels when compared to controls. Given these results it is tempting to speculate that alcohol may actually increase albumin mRNA content in man as it does in animals. Furthermore, the increased procollagen mRNA levels in fibrotic livers suggest that an increase in collagen synthesis may be a significant factor in the pathogenesis of hepatic fibrosis.

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