Use este identificador para citar ou linkar para este item: http://repositorio.ufla.br/jspui/handle/1/28488
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dc.creatorCunha, Elaine F. F. da-
dc.creatorMatos, Karina S.-
dc.creatorRamalho, Teodorico C.-
dc.date.accessioned2018-01-26T15:47:12Z-
dc.date.available2018-01-26T15:47:12Z-
dc.date.issued2013-
dc.identifier.citationCUNHA, E. F. F. da; MATOS, K. S.; RAMALHO, T. C. QSAR and docking studies of HCV NS3 serine protease inhibitors. Medicinal Chemistry, [S. l.], v. 9, n. 6, p. 774-805, 2013.pt_BR
dc.identifier.urihttp://www.eurekaselect.com/112955/articlept_BR
dc.identifier.urihttp://repositorio.ufla.br/jspui/handle/1/28488-
dc.description.abstractHepatitis C virus (HCV) is a Hepacivirus that causes chronic liver disease, leading to hepatocellular carcinoma, cirrhosis, and chronic hepatitis in about 3% of the world population. In this study, novel HCV NS3 serine protease inhibitors based on 93 boceprevir analogs were studied by QSAR analyses using thermodynamic, structural and topological descriptors, including E-state descriptors. Novel compounds were proposed using the QSAR models. Both models were highly predictive, with calibration, leave-one-out validation and external validation R2 of 0.66, 0.65 and 0.52, respectively. The most promising structures were docked into the HCV NS3 serine protease active site demonstrating, then, the high affinity of some new structures.pt_BR
dc.languageen_USpt_BR
dc.publisherBentham Sciencept_BR
dc.rightsrestrictAccesspt_BR
dc.sourceMedicinal Chemistrypt_BR
dc.subjectHepatitis C viruspt_BR
dc.subjectSerine protease inhibitorspt_BR
dc.subjectVírus da hepatite Cpt_BR
dc.subjectInibidores da serina proteasept_BR
dc.titleQSAR and docking studies of HCV NS3 serine protease inhibitorspt_BR
dc.typeArtigopt_BR
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