4.6 Article

Exploring the Synergistic Anticancer Potential of Benzofuran-Oxadiazoles and Triazoles: Improved Ultrasound- and Microwave-Assisted Synthesis, Molecular Docking, Hemolytic, Thrombolytic and Anticancer Evaluation of Furan-Based Molecules

Journal

MOLECULES
Volume 27, Issue 3, Pages -

Publisher

MDPI
DOI: 10.3390/molecules27031023

Keywords

benzofuran-oxadiazole; benzofuran-triazole; computational modeling; hemolytic activities; thrombolytic activities; anticancer activities

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Ultrasound- and microwave-assisted green synthetic strategies were used to synthesize benzofuran-oxadiazole and benzofuran-triazole derivatives. These derivatives exhibited low toxicity to red blood cells, high thrombolysis activity, and promising anticancer potential.
Ultrasound- and microwave-assisted green synthetic strategies were applied to furnish benzofuran-oxadiazole 5a-g and benzofuran-triazole 7a-h derivatives in good to excellent yields (60-96%), in comparison with conventional methods (36-80% yield). These synthesized derivatives were screened for hemolysis, thrombolysis and anticancer therapeutic potential against an A549 lung cancer cell line using an MTT assay. Derivatives 7b (0.1%) and 5e (0.5%) showed the least toxicity against RBCs. Hybrid 7f showed excellent thrombolysis activity (61.4%) when compared against reference ABTS. The highest anticancer activity was displayed by the 5d structural hybridwith cell viability 27.49 +/- 1.90 and IC50 6.3 +/- 0.7 mu M values, which were considerably lower than the reference drug crizotinib (IC50 8.54 +/- 0.84 mu M). Conformational analysis revealed the spatial arrangement of compound 5d, which demonstrated its significant potency in comparison with crizotinib; therefore, scaffold 5d would be a promising anticancer agent on the basis of cytotoxicity studies, as well as in silico modeling studies.

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