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dc.contributor.authorDasgupta, Romi
dc.contributor.authorSaha, Indraneel
dc.contributor.authorPal, Suman
dc.contributor.authorBhattacharyya, Arindam
dc.contributor.authorSa, Gaurisankar
dc.contributor.authorNag, Tapas C.
dc.contributor.authorDas, Tanya
dc.contributor.authorMaiti, B. R.
dc.date.accessioned2013-03-05T12:40:25Z
dc.date.available2013-03-05T12:40:25Z
dc.date.issued2006-10-03
dc.identifierFOR ACCESS / DOWNLOAD PROBLEM -- PLEASE CONTACT LIBRARIAN, BOSE INSTITUTE, akc@bic.boseinst.ernet.inen_US
dc.identifier.citationDasgupta R, ·saha I, Pal S, Bhattacharyya A, Sa G. Nag TC, Das T and Maiti BR. Immunosuppression. hepatotoxicity and depression of antioxidant status by arecoline. Toxicology 227:94-104, 2006.en_US
dc.identifier.issn0300-483X
dc.identifier.uri1. Full Text Link ->en_US
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dc.identifier.urihttp://www.scopus.com/record/display.url?eid=2-s2.0-33748748364&origin=resultslist&sort=plf-f&src=s&st2=Sa%2cG&nlo=&nlr=&nls=&sid=596DC08B11A1699764FDDD3E3EB034EF.WlW7NKKC52nnQNxjqAQrlA%3a1250&sot=b&sdt=b&sl=40&s=AUTHOR-NAME%28Sa%2cG%29+AND+AUTHOR-NAME%28Das%2cT%29&relpos=24&relpos=4&searchTerm=AUTHOR-NAME%28Sa%2CG%29+AND+AUTHOR-NAME%28Das%2CT%29en_US
dc.descriptionDOI: 10.1016/j.tox.2006.07.016en_US
dc.description.abstractBackground: There are about 600 million betel quid chewers in the world. Betal quid chewing is one of the major risk factors of hepatocarcinoma, oropharyngeal and esophagus cancers. Arecoline, the main Areca alkaloid of the betel nut is reported to have cytotoxic, genotoxic and mutagenic effects in various cells. It shows strong correlation to the incidence of oral submucosal fibrosis, leukoplakia and oral cancer, and has also been found to impose toxic manifestations in immune, hepatic and other defense systems of the recipient. Aim: The precise molecular mechanisms underlying the toxic effects of arecoline deserve investigation. To clarify the action of arecoline on defense systems, immune, hepatic and detoxification system were studied in mice. Method: Cell count and cell cycle of the splenocytes were studied for evaluating cell immunity. Liver function test (LFT) was followed by assaying different enzyme systems from serum (SGPT, SGOT and ALP) and liver (GST for detoxication enzyme, SOD and catalase for antioxidant enzymes and GSH for non-enzymatic antioxidant) and by ultrastructural studies of hepatocytes. Results: Here we report that arecoline arrested splenic lymphocyte cell cycle at lower concentration with induced apoptosis at higher concentration thereby causing immunosuppression in arecoline recipients. Besides, it resulted in hepatotoxicity in arecoline recipient mice by disrupting the hepatocyte ultrastructure, as judged by liver ultrastructural studies that showed decreased nuclear size, RER with profusely inflated cystemae and abundance of lipid droplets, and by up regulating hepatotoxic marker enzymes (SGOT and SGPT) in serum. Arecoline also caused depression of antioxidants, i.e., superoxide dismutase (SOD), catalase, reduced glutathione (GSH) and alutathione-S-transferase (GST) that are known to neutralize reactive oxygen species. Conclusion: All these above-mentioned results led us to conclude that arecoline attacks multiple targets to finally generate systemic toxicity in mice.en_US
dc.language.isoenen_US
dc.publisherELSEVIER IRELAND LTDen_US
dc.subjectarecolineen_US
dc.subjectcell cycleen_US
dc.subjectimmunotoxicityen_US
dc.subjecthepatotoxicityen_US
dc.subjectantioxidanten_US
dc.subjectWOS:000241258100010en_US
dc.titleImmunosuppression, hepatotoxicity and depression of antioxidant status by arecoline in albino miceen_US
dc.title.alternativeTOXICOLOGYen_US
dc.typeArticleen_US


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