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The role of N-acetylcysteine in preventing hepatic injury associated with systemic oxidative stress after extracorporeal shock wave treatment

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dc.contributor.author Baba, Dursun
dc.contributor.author Cam, Sebahat
dc.contributor.author Erdem, Havva
dc.contributor.author Senoglu, Yusuf
dc.contributor.author Yuksel, Alpaslan
dc.date.accessioned 2022-08-17T06:45:44Z
dc.date.available 2022-08-17T06:45:44Z
dc.date.issued 2020
dc.identifier.uri http://doi.org/10.17219/acem/126294
dc.identifier.uri http://earsiv.odu.edu.tr:8080/xmlui/handle/11489/2564
dc.description.abstract Background. Systemic oxidative stress may cause detrimental consequences for the liver, leading to hepatic fibrogenesis. Objectives. To investigate histopathological changes in liver tissues due to the increased systemic oxidative stress associated with rat extracorporeal shock wave lithotripsy (SWL) model and to document the consequences of N-acetylcysteine (NAC) administration. Material and methods. In this experimental SWL model, 18 Wistar albino rats were randomly assigned into 3 groups. The control group (group I) had no intervention. Group II underwent SWL treatment with intraperitonea I saline injection. Group III also had SWL with intra peritoneal NAC and was divided into short-term (group III-14 days) and long-term (group III-28 days) subgroup. Hepatectomy was performed for histopathological examinations. Histopathological alterations were evaluated with light microscopy. Immunohistological staining for p53 and myeloperoxidase was also performed. Results. Blood samples revealed a significant increase in plasma oxidative stress index (OSI) after plasma total antioxidant status (TAS) and total oxidant status (TOS) had been measured. It was shown that this increased systemic oxidative stress adversely affected liver tissues. Predominantly, sinusoidal dilatation was remarkably observed in rats with significantly high 051 values (p = 0.043). Similarly, periportal necrosis significantly increased in rats with high OSI values (p = 0.033). p53 positivity was also remarkable in rats with systemic oxidative stress (p = 0.049). N-acetylcysteine administration provided a significant decrease in OSI. N-acetylcysteine also improved all these alterations, including p53 staining. Particularly, sinusoidal dilatation was significantly protected in the long-term NAC group (group III-28 days). Conclusions. We demonstrated that SWL-induced systemic oxidative stress causes histological alterations in liver tissues. Increased p53 and myeloperoxidase staining as markers of oxidative damage were also detected. N-acetylcysteine may protect from these histological and ultra-structural alterations related to oxidative stress. en_US
dc.language.iso eng en_US
dc.publisher WROCLAW MEDICAL UNIV, UL K MARCINKOWSKIEGO 2-6, WROCLAW, 50-368, POLAND en_US
dc.relation.isversionof 10.17219/acem/126294 en_US
dc.rights info:eu-repo/semantics/openAccess en_US
dc.subject ANTIOXIDANT AGENT; INFLAMMATION; LITHOTRIPSY; DISEASES; FIBROSIS; DAMAGE en_US
dc.subject liver; oxidative stress; N-acetylcysteine; sinusoidal dilatation; p53 en_US
dc.title The role of N-acetylcysteine in preventing hepatic injury associated with systemic oxidative stress after extracorporeal shock wave treatment en_US
dc.type article en_US
dc.relation.journal ADVANCES IN CLINICAL AND EXPERIMENTAL MEDICINE en_US
dc.contributor.department Ordu Üniversitesi en_US
dc.contributor.authorID 0000-0002-3074-0240 en_US
dc.identifier.volume 29 en_US
dc.identifier.issue 10 en_US
dc.identifier.startpage 1175 en_US
dc.identifier.endpage 1180 en_US


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