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Use este identificador para citar ou linkar para este item: https://www.repositorio.mar.mil.br/handle/ripcmb/844520
Título: Design, synthesis and cytotoxicity of the antitumor agent 1-azabicycles for chemoresistant glioblastoma cells
Autor(es): Oliveira, Mona das Neves
Santana, Lourenço Luis Botelho de
Serafim, José Claudio
Santos, Airam Oliveira
Quintino, Michelle Pereira
Correia, José Tiago Menezes
Damasceno, Fabiano
Sabino, José Ricardo
Pires, Thiago Rubens Cardim
Coelho, Pedro Lucas Cerqueira
Lopes, Giselle Pinto de Faria
Ulrich, Henning
Costa, Silvia Lima
Cunha, Silvia
Palavras-chave: Saúde
Biologia
Tumores
Data do documento: 2019
Editor: Springer
Abstract: Twelve multi-functional pyrrolizidinones, indolizidinones and pyrroliazepinones were prepared from formal aza-[3 + 2] and aza-[3 + 3] cycloadditions of five- to seven-membered heterocyclic enaminones as diverse ambident electrophiles. The antitumor activity of these alkaloid-like compounds was investigated through an initial screening performed on human glioblastoma multiform (GBM) cell lines (GL-15, U251), on murine glioma cells line (C6) and on normal glial cells. Of the compounds tested, the new pyrrolo[1,2a]azepinone, [ethyl (3-oxo-1,2-diphenyl-6,7,8,9-tetrahydro-3H-pyrrolo[1,2a]azepin-9a(5H)-yl)acetate] or (Compound-13) exhibited selective cytotoxic effects on GBM-temozolomide resistant cells. Compound-13 exerted dose-dependent cytotoxic activity by promoting arrest of cells in the G0/G1 phase of the cell cycle in the first 24 h. The apoptotic effect observed was in a time-dependent manner. Anti-migratory effect promoted by the treatment with compound-13 was also observed. Moreover, healthy mixed glial cell cultures from rat brain exhibited no cytotoxicity effect upon exposure to compound-13. Thus, the present study paves the way for the use of compound-13 as novel antitumor scaffold candidate for glioma cell therapy.
Tipo de Acesso: Acesso restrito
URI: http://www.repositorio.mar.mil.br/handle/ripcmb/844520
Tipo: Artigo científico
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