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Toxicology Mechanisms and Methods Volume 26, 2016 - Issue 1
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Research Article

Angiotensin-converting enzyme inhibitor prevents oxidative stress, inflammation, and fibrosis in carbon tetrachloride-treated rat liver

Hasan Mahmud RezaDepartment of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh;Department of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh
,
Nabila TabassumDepartment of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh;Department of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh
,
Md Abu Taher SagorDepartment of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh;Department of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh
,
Mohammed Riaz Hasan ChowdhuryDepartment of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh;Department of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh
,
Mahbubur RahmanDepartment of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh;Department of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh
,
Preeti JainDepartment of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh;Department of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh
&
Md Ashraful AlamDepartment of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, Bangladesh;Department of Pharmaceutical Sciences, School of Health and Life Science, North South University Bangladesh, Bashundhara, Dhaka, BangladeshCorrespondence[email protected]
 show all
Pages 46-53 | Received 02 Mar 2015, Accepted 22 Nov 2015, Published online: 10 Feb 2016
 
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Abstract

Hepatic fibrosis is a common feature of chronic liver injury, and the involvement of angiotensin II in such process has been studied earlier. We hypothesized that anti-angiotensin II agents may be effective in preventing hepatic fibrosis. In this study, Long Evans female rats were used and divided into four groups such as Group-I, Control; Group-II, Control + ramipril; Group-III, CCl4; and Group-IV, CCl4 +ramipril. Group II and IV are treated with ramipril for 14 d. At the end of treatment, the livers were removed, and the level of hepatic marker enzymes (aspartate aminotransferase, Alanine aminotransferase, and alkaline phosphatase), nitric oxide, advanced protein oxidation product , catalase activity, and lipid peroxidation were determined. The degree of fibrosis was evaluated through histopathological staining with Sirius red and trichrome milligan staining. Carbon-tetrachloride (CCl4) administration in rats developed hepatic dysfunction and raised the hepatic marker enzymes activities significantly. CCl4 administration in rats also produced oxidative stress, inflammation, and fibrosis in liver. Furthermore, angiotensinogen-inhibitor ramipril normalized the hepatic enzymes activities and improved the antioxidant enzyme catalase activity. Moreover, ramipril treatment ameliorated lipid peroxidation and hepatic inflammation in CCl4-treated rats. Ramipril treatment also significantly reduced hepatic fibrosis in CCl4-administered rats. In conclusion, our investigation suggests that the antifibrotic effect of ramipril may be attributed to inhibition of angiotensin-II mediated oxidative stress and inflammation in liver CCl4-administered rats.

Acknowledgements

The authors gratefully acknowledge the logistic support provided by the Department of Pharmaceutical Sciences, North South University Bangladesh.

Declaration of interest

Hasan Mahmud Reza was a recipient of research grant from North South University Foundation.

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