abstract

• New derivatives of pyrroloazepinones were synthesized. The synthesis route consisted of three stages: the formation of a dimedone-derived tricarbonyl compound, the formation of a pyrrole ring resulting from the use of the Paal-Knorr method to generate tetrahydroindole-6-ones, and the expansion of the ketone by following the Schmidt method to generate lactams. The obtained 6-indolones were used to generate new derivatives: the pyrrolo[2,3-c]azepin-6-one and the pyrrolo[2,3-d]azepin-7-one ring systems. The synthesized pyrroloazepinones were evaluated for inhibitory activity in cancer cell lines and they did not show activity and cytotoxic effects on the non-tumor cells HEK239, with IC50 ≥ 215 ± 5.41 μM. ©AUTHOR(S)

authors

• Alonso-Castro A.J.
• García-Gamboa M.
• González Chávez Marco Martín
• Gámez-Gómez C.
• Martínez R.
• Miranda-Torres A.C.
• Niño Moreno Perla del Carmen
• Ávila-Zárraga J.G.

publication date

• 2020-01-01

funding provided via

• C13-FAI-03-15.15  Grant
• Consejo Nacional de Ciencia y Tecnologí­a, CONACYT: 217383  Grant
• Facultad de Ciencias Físicas y Matemáticas, FCFM  Grant
• Universidad Nacional de San Luis, UNSL  Grant
• University of Namibia, UNAM  Grant

published in

• Arkivoc  Journal

keywords

• Indolone; Pyrroloazepinone; Schmidt expansion; Wacker oxidation

Digital Object Identifier (DOI)

• 10.24820/ARK.5550190.P011.208

start page

end page

volume

• 2020

issue

• 6