Differential Effect of 4H-Benzo[d] [1, 3]oxazines on the Proliferation of Breast Cancer Cell Lines

Ixamail Fraire-Soto; Jorge Gustavo Araujo-Huitrado; Angelica Judith Granados-López; Luis A Segura-Quezada; Rafael Ortiz-Alvarado; Mayra Denise Herrera; Rosalinda Gutiérrez-Hernández; Claudia Araceli Reyes-Hernández; Yamilé López-Hernández; Melissa Tapia-Juárez; José Vicente Negrete-Díaz; Luis Chacón-García; César R Solorio-Alvarado; Jesús Adrián López

doi:10.2174/0109298673292365240422104456

Differential Effect of 4H-Benzo[d] [1, 3]oxazines on the Proliferation of Breast Cancer Cell Lines

Curr Med Chem. 2024 Apr 26. doi: 10.2174/0109298673292365240422104456. Online ahead of print.

Authors

Ixamail Fraire-Soto¹, Jorge Gustavo Araujo-Huitrado¹, Angelica Judith Granados-López¹, Luis A Segura-Quezada², Rafael Ortiz-Alvarado², Mayra Denise Herrera¹, Rosalinda Gutiérrez-Hernández¹, Claudia Araceli Reyes-Hernández¹, Yamilé López-Hernández³, Melissa Tapia-Juárez⁴, José Vicente Negrete-Díaz⁵, Luis Chacón-García⁴, César R Solorio-Alvarado², Jesús Adrián López¹

Affiliations

¹ Laboratorio de MicroRNAs y Cáncer, Universidad Autónoma de Zacatecas, Av. Preparatoria S/N, Agronómica, Campus II, Zacatecas, Zac., 98066, México.
² Universidad de Guanajuato, Campus Guanajuato, División de Ciencias Naturales y Exactas, Departamento de Química, Noria Alta S/N, 36050, Guanajuato, Guanajuato. México.
³ Laboratorio de Metabolómica y Proteómica Universidad Autónoma de Zacatecas, Av. Preparatoria S/N, Agronómica, Campus II, Zacatecas, Zac., 98066, México.
⁴ Laboratorio de Diseño Molecular, Instituto de Investigaciones Químico Biológicas, Universidad Michoacana de San Nicolás de Hidalgo, Ciudad Universitaria, Morelia, Mich., 58033, México.
⁵ Laboratory of Brain Plasticity and Integrative Neuroscience, Program of Clinical Psychology, University of Guanajuato. Guanajuato 38060, México.

PMID: 38676529
DOI: 10.2174/0109298673292365240422104456

Abstract

Background: A family of 4H-benzo[d][1,3]oxazines were obtained from a group of N-(2-alkynyl)aryl benzamides precursors via gold(I) catalysed chemoselective 6-exo-dig C-O cyclization.

Method: The precursors and oxazines obtained were studied in breast cancer cell lines MCF-7, CAMA-1, HCC1954 and SKBR-3 with differential biological activity showing various degrees of inhibition with a notable effect for those that had an aryl substituted at C-2 of the molecules. 4H-benzo[d][1,3]oxazines showed an IC50 rating from 0.30 to 157.4 µM in MCF-7, 0.16 to 139 in CAMA-1, 0.09 to 93.08 in SKBR-3, and 0.51 to 157.2 in HCC1954 cells.

Results: We observed that etoposide is similar to benzoxazines while taxol effect is more potent. Four cell lines responded to benzoxazines while SKBR-3 cell line responded to precursors and benzoxazines. Compounds 16, 24, 25 and 26 have the potent effect in cell proliferation inhibition in the 4 cell lines tested and correlated with oxidant activity suggesting a possible mechanism by ROS generation.

Conclusion: These compounds represent possible drug candidates for the treatment of breast cancer. However, further trials are needed to elucidate its full effect on cellular and molecular features of cancer.

Keywords: Benzoxazines; Breast Cancer; Cell Lines; Oxidation; Proliferation; Reduction..