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dc.contributor.authorRodrigues, Felipe A. R.-
dc.contributor.authorBomfim, Igor da S.-
dc.contributor.authorCavalcanti, Bruno C.-
dc.contributor.authorPessoa, Claudia-
dc.contributor.authorGoncalves, Raoni S. B.-
dc.contributor.authorWardell, James L.-
dc.contributor.authorWardel, Solange M. S. V.-
dc.contributor.authorSouza, Marcus V. N. de-
dc.date.accessioned2014-02-07T11:52:16Z-
dc.date.available2014-02-07T11:52:16Z-
dc.date.issued2014-
dc.identifier.citationRODRIGUES, F. A. R. et al. Mefloquine–Oxazolidine derivatives : a new class of anticancer agents. Chemical Biology & Drug Design, Oxford, Inglaterra, v. 83, n. 1, p. 126-131, 2014.pt_BR
dc.identifier.issn1747-0277-
dc.identifier.urihttp://www.repositorio.ufc.br/handle/riufc/7215-
dc.description.abstractA series of 23 racemic mefloquine–oxazolidine derivatives, 4-[3-(aryl)hexahydro[1,3]oxazolo[3,4-a]pyridin- 1-yl]-2,8-bis(trifluoromethyl)quinolines, derived from (R*, S*)-(±)-mefloquine and arenealdehydes, have been evaluated for their activity against four cancer cell lines (HCT-8, OVCAR-8, HL-60, and SF-295). Good cytotoxicities have been determined with IC50 values ranging from 0.59 to 4.79 lg/mL. In general compounds with aryl groups having strong electron-releasing substituents, such as HO and MeO, or electron-rich heteroaryl groups, for example imidazol-2-y-l, are active. However, other factors such as steric effects may play a role. As both the active and non-active conformations of the mefloquine–oxazolidine derivatives are similar, it is concluded that molecular conformations do not play a significant role either. This study is the first to evaluate mefloquine derivatives as antitumor agents. The mefloquine–oxazolidine derivatives are considered to be useful leads for the rational design of new antitumor agents.pt_BR
dc.language.isoenpt_BR
dc.publisher1747-0277pt_BR
dc.subjectMefloquinapt_BR
dc.titleMefloquine–Oxazolidine derivatives : a new class of anticancer agentspt_BR
dc.typeArtigo de Periódicopt_BR
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