Abstract
Drug-induced hepatotoxicity is a frequent cause of liver injury worldwide. The present study was designed to evaluate the possible hepato-protective potential Agaricus bisporus extract (ABE; a type of mushrooms) in albino rats using Carbon tetrachloride (CCl4)-model of liver injury. Forty-two albino rats were utilized in this experiment arranged randomly in seven groups, six rats each, of different treatments. He-patic injury model was induced by administration of CCl4 (25% in corn oil) at a dose of 2.5 ml/kg, interperitoneally, twice weekly for 8 weeks (+ve control); test group rats received ABE at escalating doses of 200 or 400 mg/kg, orally, daily for 8 weeks with exposure to CCl4; standard group rats received Silymarin at dose of 100 mg/kg, orally, daily for 8 weeks along with CCl4; further 2 groups of rats received only ABE at the same dose levels; while rats of -ve control group received only the vehicles of the used drugs. Blood and liver tissue sam-ples were picked out at the end of the experimental course for different assays. Biochemical analysis revealed that ABE exhibited dose-dependent hepatoprotection indicated by almost normalized biomarkers, including, enzymatic liver function parameters, namely, AST, ALT, GGT & ALP with potential % of 93.1, 58.2, 65.2, 68.9, respectively, after ABE large dose when standardized by Silymarin; non-enzymatic parameters, namely, total protein, albumin, globulins, total bilirubin, conjugated bilirubin, unconjugated bilirubin, TAGs, Cholesterol, HDL, LDL & VLDL with potential % of 59.3, 54.5, 57.3, 81.8, 81.0, 80.0, 75.5, 90.4, 80.8, 84.5 & 78.7, respectively, after ABE large dose when standardized by Silymarin. The mechanism of the obtained hepatoprotection of ABE may be based on impeding the oxidative stress mediated by the used hepatotoxin, indicated by reduced MDA (37.9 % of Silymarin), and restored SOD, Catalase & GPx in liver homogenate with potentials of 94.9, 63.0 & 88.4 % of Silymarin, respectively. Pathological findings, both macroscopic and microscopic, were supportive to the biochemical findings, where the pathological lesions caused by CCl4 as fatty degeneration of hepatocytes with vacuolated cytoplasm, proliferated fibrous connective tissue with eosinophilic edematous fluid cells plus focal and diffuse necrotic areas and hyperplastic biliary epithelium, were ameliorated dose-dependently when ABE was administered together with CCl4. Data of the present study may suggest ABE as a good natural source for promising hepatoprotective and antioxidative remedies.
Highlights
The Liver is vital organ and plays important role in drug metabolism
Drug-induced hepatotoxicity is a frequent cause of liver injury in Egypt and developed countries who are suffering from various complications in the liver (Omar et al 2013)
The aim of the present study was to evaluate the hepatoprotective properties of mushroom extract (Agaricus bisporus extract, ABE) in context of its antioxidant properties
Summary
The Liver is vital organ and plays important role in drug metabolism. Using a lot of drugs increases risk of liver injury. Using a prospective, population-based French study with an annual estimated incidence of 13.9 ± 2.4 drug induced liver injury (DILI) cases per 100,000 inhabitants, it has been extrapolated that nearly 44,000 individuals in the United States will suffer from DILI each year (Bell & Chalasani 2009). The aim of the present study was to evaluate the hepatoprotective properties of mushroom extract (Agaricus bisporus extract, ABE) in context of its antioxidant properties To achieve this aim, the following objectives have been investigated: liver enzymatic markers in plasma as AST, ALT, GGT, ALP; liver non-enzymatic parameters in plasma as proteins, bilirubins, triglycerides, cholesterol and lipoproteins; oxidative stress markers in liver homogenate as MDA, superoxide dismutase, catalase and glutathione peroxidase; pathological examination of the liver both macroscopic and microscopic
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More From: International Journal of Pharmacology and Toxicology
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