Hepatic cirrhosis induced by thioacetamide: study of the model of intraperitoneal long term administration in Wistar rats

The low sensitivity of animals to drugs and the lack of changes in liver function are the main difficulties for the development of experimental liver cirrhosis. The aim of this study was improving the model of cirrhosis by intraperitoneal injection of thioacetamide (TAA) to reduce the animal adaptation to the drug. We used 5 groups of female Wistar rats: A (200 mg TAA/kg), B (increase of 20% to 48 days), C (increase of 10% every 24 days), D (increase of 15% every 24 days), E (saline). The animals were injected 3 times a week for 14 weeks. Blood samples were collected by cardiac puncture at the start and at the end of the experiment as well as before each dose increment, for analysis of markers of liver function. The behavioral assessment was done by the method of elevated plus-maze. Samples of liver were collected and processed to light microscopy. The animals treated with TAA showed piloerection, jaundice and chromodacryorrhea. Behavioral test showed stress and/or anxiety in these animals. The liver cirrhosis showed regenerative nodules and hemorrhagic lesions on the surface. Weight gain was similar among the groups treated, however, all of them were smaller than those of group E. The damage of the liver function was more pronounced in groups where the dose was increased over the experimental period, however, the mortality of group D was higher (44%). Treatment with TAA led to the development of cirrhosis with formation of regenerative nodules surrounded by fibrous septa and hepatic architecture disruption. The deposition of collagen was higher in groups B and C, whereas group D was similar to group A. Histopathologic evaluation showed intense proliferation of oval cells and bile duct hyperplasia, with production of acid mucin. It was observed the presence of hemosiderin, hepatocyte ballonization, nuclear lesions and inflammatory cells. The administration of TAA led to the development of neoplastic lesions, suggesting possible carcinogenic effect of this substance. The results showed that the treatment of groups B and C were most effective in the development of experimental cirrhosis. Despite that animals of group D received an increment in their TAA dose, their results seems similar to those of group A but with high mortality, probably because the treatment selected resistant animals to the drug. Therefore, it is recommended the model of induction of group B due to the lower mortality (5%), less influence on the emotional aspect and development of cirrhosis as severe as that the rats of group C. (AU)