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Journal of Investigative Surgery Volume 28, 2015 - Issue 5: Advances in Ischemia and Reperfusion
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ORIGINAL ARTICLE

Nebivolol Ameliorates Hepatic Ischemia/Reperfusion Injury on Liver But Not on Distant Organs

Burak Veli UlgerDepartment of General Surgery, Dicle University Medical Faculty, Diyarbakır, TurkeyCorrespondence[email protected]
,
Halil ErbisDepartment of General Surgery, Akdeniz University Medical Faculty, Antalya, Turkey
,
Gul TurkcuDepartment of Pathology, Dicle University Medical Faculty, Diyarbakır, Turkey
,
Aysun EkinciDepartment of Biochemistry, Dicle University Medical Faculty, Diyarbakır, Turkey
,
Mehmet Akif TurkogluDepartment of General Surgery, Akdeniz University Medical Faculty, Antalya, Turkey
,
Cenap EkinciDepartment of Histology, Dicle University Medical Faculty, Diyarbakır, Turkey
,
Vural Taner YilmazDepartment of Internal Medicine, Akdeniz University Medical Faculty, Antalya, Turkey
&
Bilsel BacDepartment of General Surgery, Dicle University Medical Faculty, Diyarbakır, Turkey
 show all
Pages 245-252 | Received 30 Dec 2014, Accepted 17 Mar 2015, Published online: 25 Aug 2015
 
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ABSTRACT

Introduction: Hepatic ischemia/reperfusion injury may occur after large tumor resection and liver transplantation procedures. Nitric oxide was shown to have protective effects on ischemia/reperfusion injury. Nebivolol is a compound that has been reported to improve nitric oxide release. We evaluated the effects of nebivolol in a rat liver ischemia/reperfusion model. Methods: A total of 40 rats were randomly divided into four groups (n = 10 each). Group I underwent only laparotomy, Group II was administered nebivolol and then underwent laparotomy, Group III underwent laparotomy and hepatic ischemia/reperfusion, and Group IV was administered nebivolol and then underwent laparotomy and hepatic ischemia/reperfusion. Serum AST, ALT, urea, and creatinine levels, and TAS and TOS levels of liver, lung, and kidney tissues were determined. Histopathological determination was also performed. Results: Nebivolol significantly reduced liver function tests in group IV, but it did not improve renal functions. Oxidative stress and abnormal histopathological findings were found to be reduced in liver tissue in group IV. Although the oxidative stress was increased after hepatic ischemia/reperfusion, nebivolol could not reduce the oxidative stress in kidney tissue. There were no significant differences between group III and group IV in terms of the histopathological changes in kidney tissue. There were no significant differences in lung tissue between the groups. Conclusions: The results of this study suggest that nebivolol has protective effects on liver but not on distant organs in a hepatic ischemia/reperfusion injury model. These experimental findings indicate that nebivolol may be useful in the treatment of hepatic ischemia/reperfusion injury.

This study was financially supported by Dicle University, Coordination of Scientific Research Projects (Project no: 13-TF-97).

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