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Open Access@KRIBBJeonbuk Branch InstituteFunctional Biomaterial Research Center1. Journal Articles

Melatonin improves adriamycin-induced hepatic oxidative damage in rats

Cited 6 time in scopus
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dc.contributor.authorIn Chul Lee-
dc.contributor.authorS H Kim-
dc.contributor.authorH S Baek-
dc.contributor.authorC Moon-
dc.contributor.authorC S Bae-
dc.contributor.authorS H Kim-
dc.contributor.authorWoon Kee Yoon-
dc.contributor.authorKi Hoan Nam-
dc.contributor.authorHyoung-Chin Kim-
dc.contributor.authorJ C Kim-
dc.date.accessioned2017-04-19T09:45:19Z-
dc.date.available2017-04-19T09:45:19Z-
dc.date.issued2013-
dc.identifier.issnI000-0184-
dc.identifier.uri10.1007/s13273-013-0033-0ko
dc.identifier.urihttps://oak.kribb.re.kr/handle/201005/11583-
dc.description.abstractThe present study investigated the possible ameliorative effects of melatonin (MLT) against adriamycin (ADR)-induced hepatotoxicity and oxidative stress in rats. The following four experimental groups were evaluated: (1) vehicle control, (2) MLT (15 mg/kg/day), (3) ADR (10 mg/kg), and (4) ADR&MLT. ADR caused severe hepatotoxicity as evidenced by an elevation of serum aspartate aminotransferase and alanine aminotransferase activities, increased total bilirubin concentration, and decreased albumin and total protein concentration, indicating hepatic function abnormalities. Histopathological examination revealed various structural changes in liver, characterized by hepatocyte degeneration/necrosis, congestion, sinusoidal dilatation, vacuolation, and inflammatory cell infiltration. The significant decrease in reduced glutathione (GSH) content, catalase, superoxide dismutase (SOD), glutathione peroxidase (GPx), and glutathione reductase (GR) activities and the significant increase in malondialdehyde (MDA) content indicated that ADR-induced hepatotoxicity was mediated through oxidative stress. In contrast, MLT treatment significantly improved ADR-induced serum biochemical and histo-pathological alterations reflecting hepatic dysfunction. Moreover, MDA concentration and GSH content, GR, GPx, and SOD activities were not affected when MLT was administered in conjunction with ADR. These results indicated that MLT improved the oxidative damage induced by ADR in rat liver, presumably due to its ability to inhibit lipid peroxidation, and restore both enzymatic and nonenzymatic antioxidant activities.-
dc.publisherKorea Soc-Assoc-Inst-
dc.titleMelatonin improves adriamycin-induced hepatic oxidative damage in rats-
dc.title.alternativeMelatonin improves adriamycin-induced hepatic oxidative damage in rats-
dc.typeArticle-
dc.citation.titleMolecular & Cellular Toxicology-
dc.citation.number3-
dc.citation.endPage265-
dc.citation.startPage257-
dc.citation.volume9-
dc.contributor.affiliatedAuthorIn Chul Lee-
dc.contributor.affiliatedAuthorWoon Kee Yoon-
dc.contributor.affiliatedAuthorKi Hoan Nam-
dc.contributor.affiliatedAuthorHyoung-Chin Kim-
dc.contributor.alternativeName이인철-
dc.contributor.alternativeName김성환-
dc.contributor.alternativeName백형선-
dc.contributor.alternativeName문창종-
dc.contributor.alternativeName배천식-
dc.contributor.alternativeName김성호-
dc.contributor.alternativeName윤원기-
dc.contributor.alternativeName남기환-
dc.contributor.alternativeName김형진-
dc.contributor.alternativeName김종춘-
dc.identifier.bibliographicCitationMolecular & Cellular Toxicology, vol. 9, no. 3, pp. 257-265-
dc.identifier.doi10.1007/s13273-013-0033-0-
dc.subject.keywordAdriamycin-
dc.subject.keywordHepatotoxicity-
dc.subject.keywordMelatonin-
dc.subject.keywordOxidative stress-
dc.subject.keywordProtective effects-
dc.subject.localAdriamycin-
dc.subject.localhepatotoxicity-
dc.subject.localHepatotoxicity-
dc.subject.localMelatonin-
dc.subject.localmelatonin-
dc.subject.localOxidative stre-
dc.subject.localOxidative stress-
dc.subject.localOXIDATIVE STRESS-
dc.subject.localOxidative Stress-
dc.subject.localoxidative stress-
dc.subject.localprotective effects-
dc.subject.localProtective effects-
dc.subject.localprotective effect-
dc.subject.localProtective effect-
dc.description.journalClassY-
Appears in Collections:
Jeonbuk Branch Institute > Functional Biomaterial Research Center > 1. Journal Articles
Ochang Branch Institute > Division of National Bio-Infrastructure > Laboratory Animal Resource & Research Center > 1. Journal Articles
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