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Oncostatin M Gene Therapy Attenuates Liver Damage Induced by Dimethylnitrosamine in Rats

机译:抑癌素M基因疗法可减轻二甲基亚硝胺对大鼠肝脏的损害

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To assess the usefulness of oncostatin M (osm) gene therapy in liver regeneration, we examined whether the introduction of OSM cDNA enhances the regeneration of livers damaged by dimethylnitrosamine (DMN) in rats. Repeated injection of OSM cDNA enclosed in hemagglutinating virus of Japan envelope into the spleen resulted in the exclusive expression of OSM protein in Kupffer cells of the liver, which was accompanied by increases in body weight, liver weight, and serum albumin levels and the reduction of serum liver injury parameters (bilirubin, aspartate aminotransferase, and alanine aminotransferase) and a serum fibrosis parameter (hyaluronic acid). Histological examination showed that osm gene therapy reduced centrilobular necrosis and inflammatory cell infiltration and augmented hepatocyte proliferation. The apoptosis of hepatocytes and fibrosis were suppressed by osm gene therapy. Time-course studies on osm gene therapy before or after DMN treatment showed that this therapy was effective not only in enhancing regeneration of hepatocytes damaged by DMN but in preventing hepatic cytotoxicity caused by subsequent treatment with DMN. These results indicate that OSM is a key mediator for proliferation and anti-apoptosis of hepatocytes and suggest that osm gene therapy is useful, as preventive and curative means, for the treatment of patients with liver damage.
机译:为了评估抑癌素M(osm)基因疗法在肝脏再生中的有用性,我们检查了OSM cDNA的引入是否增强了被二甲基亚硝胺(DMN)损伤的大鼠肝脏的再生。将日本血凝病毒包膜中封闭的OSM cDNA重复注射到脾脏中导致OSM蛋白在肝脏的Kupffer细胞中排他性表达,并伴随着体重,肝脏重量和血清白蛋白水平的增加以及血清白蛋白水平的降低。血清肝损伤参数(胆红素,天冬氨酸转氨酶和丙氨酸转氨酶)和血清纤维化参数(透明质酸)。组织学检查显示,osm基因疗法可减少小叶坏死和炎性细胞浸润,并增强肝细胞增殖。渗透基因治疗抑制了肝细胞的凋亡和纤维化。在DMN治疗之前或之后进行的osm基因疗法的时程研究表明,这种疗法不仅有效增强了DMN损伤的肝细胞的再生,而且还有效地防止了DMN后续治疗引起的肝细胞毒性。这些结果表明,OSM是肝细胞增殖和抗凋亡的关键介质,并表明osm基因疗法作为预防和治疗手段,对于治疗肝损伤患者是有用的。

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