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Please use this identifier to cite or link to this item: http://acervodigital.unesp.br/handle/11449/74102
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dc.contributor.authorAssumpção, Juliana Uruguay Correa Vidigal-
dc.contributor.authorCampos, Michel Leandro-
dc.contributor.authorFerraz Nogueira Filho, Marco Antonio-
dc.contributor.authorPestana, Kelly Chrystina-
dc.contributor.authorBaldan, Helen Mariana-
dc.contributor.authorFormariz Pilon, Thalita Pedroni-
dc.contributor.authorOliveira, Anselmo Gomes de-
dc.contributor.authorPeccinini, Rosangela Goncalves-
dc.date.accessioned2014-05-27T11:27:26Z-
dc.date.accessioned2016-10-25T18:40:44Z-
dc.date.available2014-05-27T11:27:26Z-
dc.date.available2016-10-25T18:40:44Z-
dc.date.issued2013-01-01-
dc.identifierhttp://dx.doi.org/10.1002/jps.23368-
dc.identifier.citationJournal of Pharmaceutical Sciences, v. 102, n. 1, p. 289-296, 2013.-
dc.identifier.issn0022-3549-
dc.identifier.issn1520-6017-
dc.identifier.urihttp://hdl.handle.net/11449/74102-
dc.identifier.urihttp://acervodigital.unesp.br/handle/11449/74102-
dc.description.abstractDoxorubicin (DOX) is an anthracycline antibiotic with a broad antitumor spectrum. However, the clinical use of DOX is limited because of its cardiotoxicity, a dose-dependent effect. Colloidal drug delivery systems, such as microemulsions (MEs), allow the incorporation of drugs, modifying the pharmacokinetic (PK) profile and toxic effects. In this study, we evaluated the PK profile and cardiotoxicity of a new DOX ME (DOX-ME). The PK profile of DOX-ME was determined and compared with that of the conventional DOX after single-dose administration (6mg/kg, intravenous) in male Wistar rats (n = 12 per group). The cardiotoxicity of DOX formulations was evaluated by serum creatine kinase MB (CKMB) activity in both animal groups before and after drug administration. The plasma DOX measurements were performed by high-performance liquid chromatography with fluorescence detection, and the CKMB levels were assayed using the CKMB Labtest® kit. The ME system showed a significant increase in plasma DOX concentrations and lower distribution volume when compared with conventional DOX. Serum CKMB activity increased after conventional DOX administration but was unchanged in the DOX-ME group. These results demonstrate modifications in drug access to susceptible sites using DOX-ME. DOX-ME displayed features that make it a promising system for future therapeutic application. © 2012 Wiley Periodicals, Inc.en
dc.format.extent289-296-
dc.language.isoeng-
dc.sourceScopus-
dc.subjectBiocompatible microemulsion-
dc.subjectCancer chemotherapy-
dc.subjectCardiotoxicity-
dc.subjectCKMB-
dc.subjectDistribution-
dc.subjectDoxorubicin-
dc.subjectHPLC (High-Performance/Pressure-Liquid-Chromatography)-
dc.subjectPharmacokinetics-
dc.subjectToxicology-
dc.subjectcreatine kinase MB-
dc.subjectdoxorubicin-
dc.subjectanimal experiment-
dc.subjectanimal model-
dc.subjectbiocompatibility-
dc.subjectblood sampling-
dc.subjectcardiotoxicity-
dc.subjectdrug blood level-
dc.subjectdrug formulation-
dc.subjectenzyme activity-
dc.subjectfluorescence analysis-
dc.subjecthigh performance liquid chromatography-
dc.subjectmale-
dc.subjectmicroemulsion-
dc.subjectnonhuman-
dc.subjectrat-
dc.subjectsingle drug dose-
dc.subjectAnimals-
dc.subjectAntibiotics, Antineoplastic-
dc.subjectBiological Markers-
dc.subjectChemistry, Pharmaceutical-
dc.subjectChromatography, High Pressure Liquid-
dc.subjectCreatine Kinase, MB Form-
dc.subjectEmulsions-
dc.subjectHeart Diseases-
dc.subjectInjections, Intravenous-
dc.subjectLipids-
dc.subjectMale-
dc.subjectRats-
dc.subjectRats, Wistar-
dc.subjectTechnology, Pharmaceutical-
dc.titleBiocompatible microemulsion modifies the pharmacokinetic profile and cardiotoxicity of doxorubicinen
dc.typeoutro-
dc.contributor.institutionUniversidade Estadual Paulista (UNESP)-
dc.contributor.institutionUniversity Center of Araraquara, UNIARA-
dc.description.affiliationSchool of Pharmaceutical Sciences Sao Paulo State University, UNESP, Araraquara 14801-902, SP-
dc.description.affiliationDentistry Post Graduation Course University Center of Araraquara, UNIARA, Araraquara 14807-120, SP-
dc.description.affiliationUnespSchool of Pharmaceutical Sciences Sao Paulo State University, UNESP, Araraquara 14801-902, SP-
dc.identifier.doi10.1002/jps.23368-
dc.identifier.wosWOS:000312145900030-
dc.rights.accessRightsAcesso restrito-
dc.relation.ispartofJournal of Pharmaceutical Sciences-
dc.identifier.scopus2-s2.0-84870714526-
Appears in Collections:Artigos, TCCs, Teses e Dissertações da Unesp

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