Please use this identifier to cite or link to this item: http://earsiv.odu.edu.tr:8080/xmlui/handle/11489/2395
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dc.contributor.authorAtmaca, Hasan T.-
dc.contributor.authorCadirci, Elif-
dc.contributor.authorHalici, Zekai-
dc.contributor.authorKarakus, Emre-
dc.contributor.authorKaraman, Adem-
dc.contributor.authorKunak, Celalettin S.-
dc.contributor.authorPolat, Beyzagul-
dc.contributor.authorSaritemur, Murat-
dc.contributor.authorUgan, Rustem A.-
dc.contributor.authorUn, Harun-
dc.date.accessioned2022-08-17T05:46:57Z-
dc.date.available2022-08-17T05:46:57Z-
dc.date.issued2016-
dc.identifier.urihttp://doi.org/10.1259/bjr.20140724-
dc.identifier.urihttps://www.birpublications.org/doi/10.1259/bjr.20140724-
dc.identifier.urihttp://earsiv.odu.edu.tr:8080/xmlui/handle/11489/2395-
dc.description.abstractObjective: Contrast media (CM) are a major cause of nephropathy in high-risk patients. The aim of this study was to examine the effects of carnitine (CAR) in advanced nephrotoxicity due to CM administration in rats with glycerol-induced renal functional disorder. Methods: 40 rats were divided randomly into five groups (n=8): (1) healthy group; (2) glycerol only (GLY); (3) glycerol and CM (GLY1CM); (4) glycerol, CM and 200 mg kg(-1) carnitine (CAR200, Carnitene (R); Sigma-tau/Santa Farma, Istanbul, Turkey); and (5) glycerol, CM and 400 mg kg(-1) carnitine (CAR400). Kidney injury was induced with a single-dose, intramuscular injection of 10 ml kg(-1) body weight (b.w.) of GLY. CAR was administered intraperitoneally. CM (8 ml kg(-1) b.w. iohexol, Omni-paque (TM) T; Opakim Medical Products, Istanbul, Turkey) was infused via the tail vein to the rats in Groups 3-5. Results: L-carnitine administration significantly decreased serum creatinine and blood urea nitrogen levels. Superoxide dismutase and glutathione activity increased significantly in the treatment groups compared with the nephrotoxic groups. CAR400 significantly reduced malondialdehyde levels to healthy levels. In the treatment groups, tumour necrosis factor (TNF)-beta, transforming growth factor 1 beta, interleukin 1 beta and caspase-3 gene expression decreased compared with the nephrotoxic groups. TNF-alpha and nuclear factor kappa-beta (NF-kappa B) protein expression increased after CM and CAR administration reduced both TNF-alpha and NF-kappa B expressions. Histopathologically, hyaline and haemorrhagic casts and necrosis in proximal tubules increased in the nephrotoxicity groups and decreased in the CAR groups. Conclusion: The results reveal that L-carnitine protects the oxidant/antioxidant balance and decreases proinflammatory cytokines and apoptosis in CM-induced nephrotoxicity in rats with underlying pathology. Advances in knowledge: Depending on the underlying kidney pathologies, the incidence of CM-induced nephropathy (CIN) increases. Therefore, this is the best model to represent clinically observed CIN. Advances in knowledge: Depending on the underlying kidney pathologies, the incidence of CM-induced nephropathy (CIN) increases. Therefore, this is the best model to represent clinically observed CIN.en_US
dc.language.isoengen_US
dc.publisherBRITISH INST RADIOLOGY, 36 PORTLAND PLACE, LONDON W1N 4AT, ENGLANDen_US
dc.relation.isversionof10.1259/bjr.20140724en_US
dc.rightsinfo:eu-repo/semantics/openAccessen_US
dc.subjectCISPLATIN-INDUCED NEPHROTOXICITY; ENHANCED COMPUTED-TOMOGRAPHY; MEDIA-INDUCED NEPHROPATHY; FACTOR-KAPPA-B; TNF-ALPHA; TGF-BETA; RADIOCONTRAST NEPHROPATHY; RISK STRATIFICATION; N-ACETYLCYSTEINE; EPITHELIAL-CELLSen_US
dc.titleNephroprotective potential of carnitine against glycerol and contrast-induced kidney injury in rats through modulation of oxidative stress, proinflammatory cytokines, and apoptosisen_US
dc.typearticleen_US
dc.relation.journalBRITISH JOURNAL OF RADIOLOGYen_US
dc.contributor.departmentOrdu Üniversitesien_US
dc.contributor.authorID0000-0001-8379-4114en_US
dc.contributor.authorID0000-0002-0822-0054en_US
dc.contributor.authorID0000-0002-3091-0609en_US
dc.contributor.authorID0000-0002-4837-2343en_US
dc.contributor.authorID0000-0003-0836-7205en_US
dc.contributor.authorID0000-0003-1772-282Xen_US
dc.contributor.authorID0000-0003-2042-5949en_US
dc.contributor.authorID0000-0003-2231-3967en_US
dc.identifier.volume89en_US
dc.identifier.issue1058en_US
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