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KMID : 1161420150180030290
Journal of Medicinal Food
2015 Volume.18 No. 3 p.290 ~ p.298
Silymarin Inhibits the Progression of Fibrosis in the Early Stages of Liver Injury in CCl4-Treated Rats
Clichici Simona

Olteanu Diana
Nagy Andras-Laszlo
Oros Adrian
Filip Adriana
Mircea Petru A.
Abstract
Liver fibrosis, a common condition occurring during the evolution of almost all chronic liver diseases, is the consequence of hepatocyte injury that leads to the activation of Kupffer cells and hepatic stellate cells (HSC). Silymarin (Si) is a herbal product widely used for its hepatoprotective potential. Our study aims to investigate the effects of two different doses of Silymarin on a CCl4-induced model of liver fibrosis with a focus on the early stages of liver injury. Fifty Wistar rats were randomly divided into five groups (n=10): control group (sunflower oil twice a week); CMC group (carboxymethyl cellulose five times a week, sunflower oil twice a week); CCl4 group (CCl4 in sunflower oil, by gavage, twice a week); CCl4+Si 50 group (CCl4 twice a week, Silymarin 50?mg/b.w. in CMC five times a week); and CCl4+Si 200 group (similar to the previous group, with Si 200?mg/b.w.). One month after the experiment began we explored hepato-cytolysis (aminotransferases and lactate dehydrogenase), oxidative stress, fibrosis (histological score, hyaluronic acid), markers of HSC activation (transforming growth factor ¥â1 [TGF-¥â1], and ¥á-smooth muscle actin [¥á-SMA] expression by western blot) and activation of Kupffer cells by immunohistochemistry. Our data showed that Si 50?mg/b.w. had the capacity of reducing oxidative stress, hepato-cytolysis, fibrosis, activation of Kupffer cells, and the expression of ¥á-SMA and TGF-¥â1 with better results than Si 200?mg/b.w. Thus, the usual therapeutic dose of Silymarin, administered in the early stages of fibrotic changes is capable of inhibiting the fibrogenetic mechanism and the progression of initial liver fibrosis.
KEYWORD
liver fibrosis, oxidative stress, Silymarin
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