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Pirfenidone effectively reverses experimental liver fibrosis.

机译:吡非尼酮可有效逆转实验性肝纤维化。

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摘要

BACKGROUND/AIMS: Our group has been involved in searching for different strategies to ameliorate hepatic cirrhosis. The aim of this study was to evaluate the effect of Pirfenidone in the reversion or prevention of cirrhosis experimentally induced in rats by chronic administration of CCl(4) and bile-duct ligation (BDL). METHODS: Male cirrhotic Wistar rats (8 weeks of intoxication and then hepatotoxin was discontinued) received either oral saline or Pirfenidone at 500 mg/kg per day. RESULTS: High levels of alanine aminotransferase, aspartate aminotransferase, and alkaline phosphatase decreased significantly (P<0.001) in animals treated with Pirfenidone (n=11) with regard to saline-administrated animals (n=9). Prothrombin activity and bilirubins were also reduced. Computerized fibrosis index demonstrated a 70% decrease (P<0.001) along with less hydroxyproline content, reduction in activated HSC and higher active cell regeneration. A rearrangement of the parenchyma was also noted and gene expression of collagens I, III and IV, transforming growth factor beta-1, Smad-7, TIMP-1 and PAI-1 decreased considerably in treated animals. Cirrhotic rats in which CCl(4) was not discontinued displayed 40% liver fibrosis reduction. In a different cirrhosis model, 4-week BDL rats treated with the drug showed a significant 50% reduction in hepatic fibrosis (P<0.01). CONCLUSIONS: This new drug might be useful in healing human disease.
机译:背景/目的:我们的研究小组一直致力于寻找改善肝硬化的不同策略。这项研究的目的是评估吡非尼酮在慢性给药CCl(4)和胆管结扎术(BDL)中对大鼠实验性逆转或预防肝硬化的作用。方法:雄性肝硬化Wistar大鼠(中毒8周,然后停用肝毒素)每天口服500 mg / kg的盐水或吡非尼酮。结果:相对于盐水给药的动物(n = 9),用吡非尼酮(n = 11)治疗的动物中高水平的丙氨酸氨基转移酶,天冬氨酸氨基转移酶和碱性磷酸酶显着降低(P <0.001)。凝血酶原活性和胆红素也降低。计算机化纤维化指数显示降低70%(P <0.001),同时羟脯氨酸含量降低,活化的HSC降低和活性细胞再生更高。还注意到实质的重排,并且在治疗的动物中,胶原蛋白I,III和IV,转化生长因子β-1,Smad-7,TIMP-1和PAI-1的基因表达显着降低。没有停止CCl(4)的肝硬化大鼠肝纤维化减少40%。在另一种肝硬化模型中,用该药物治疗的4周BDL大鼠肝纤维化明显降低了50%(P <0.01)。结论:这种新药可能对治愈人类疾病有用。

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