Please use this identifier to cite or link to this item: http://earsiv.odu.edu.tr:8080/xmlui/handle/11489/2449
Title: The Effect of Etoricoxib on Hepatic Ischemia-Reperfusion Injury in Rats
Authors: Alp, Hamit Hakan
Altuner, Durdu
Binici, Orhan
Genc, Fatma
Kukula, Osman
Kunak, Celalettin Semih
Kuyrukluyildiz, Ufuk
Mutlu, Emre
Peker, Gulcer Gulec
0000-0001-7244-0281
0000-0002-3158-8252
0000-0002-9202-4944
0000-0003-2231-3967
Keywords: OXIDATIVE DNA-DAMAGEISCHEMIA/REPERFUSION INJURYBIOLOGICAL-FLUIDSNITRIC-OXIDEASSAYPREVENTIONTISSUEDRUGS
Issue Date: 2015
Publisher: HINDAWI LTDADAM HOUSE, 3RD FLR, 1 FITZROY SQ, LONDON W1T 5HF, ENGLAND
Abstract: Ischemia-reperfusion (I/R) damage is known to be a pathological process which continues with the increase of oxidants and expands with the inflammatory response. There is not any study about protective effect of etoricoxib on the liver I/R damage in literature. Objective. This study investigates the effect of etoricoxib on oxidative stress induced by I/R of the rat liver. Material and Methods. Experimental animals were divided into four groups as liver I/R control (LIRC), 50 mg/kg etoricoxib + liver I/R (ETO-50), 100 mg/kg etoricoxib + liver I/R (ETO-100), and healthy group (HG). ETO-50 and ETO-100 groups were administered etoricoxib, while LIRC and HG groups were orally given distilled water by gavage. Hepatic artery was clamped for one hour to provide ischemia, and then reperfusion was provided for 6 hours. Oxidant, antioxidant, and COX-2 gene expressions were studied in the liver tissues. ALT and AST were measured. Results. Etoricoxib in 50 and 100 mg/kg doses changed the levels of oxidant/antioxidant parameters such as MDA, MPO, tGSH, GSHRd, GST, SOD, NO, and 8-OH/Gua in favour of antioxidants. Furthermore, etoricoxib prevented increase of COX-2 gene expression and ALT and AST levels. This important protective effect of etoricoxib on the rat liver I/R can be tested in the clinical setting.
URI: http://doi.org/10.1155/2015/598162
http://earsiv.odu.edu.tr:8080/xmlui/handle/11489/2449
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