Design, synthesis, biological evaluation and in silico studies of 2-anilino- 4-(benzimidazol- 1-yl)pyrimidine scaffold as antitumor agents

Design, synthesis, biological evaluation and in silico studies of 2-anilino- 4-(benzimidazol- 1-yl)pyrimidine scaffold as antitumor agents

Abstract In an attempt to rationalize the search for new potential Chemotherapeutic agents, a new series of 2-anilinobenzimidazol derivatives with CDK activity have been synthesized. The newly synthesized compounds have been assessed for their cytotoxic effects and CDK activity. These presented comp...

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Bibliographic Details
Main Authors: Lamees S. Al-Rasheed, Siddique Akber Ansari, Hanadi H. Asiri, Ahmed H. Bakheit, Abdulrahman A. Al-mehizia, Amsha S. Alsegiani, Hamad M. Alkahtani
Format: Article
Language:English
Published: Springer 2025-05-01
Series:Saudi Pharmaceutical Journal
Subjects:
Cancer
Benzimidazole
CDK
Antitumor activity
Molecular docking
Online Access:https://doi.org/10.1007/s44446-025-00010-w
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Summary:Abstract In an attempt to rationalize the search for new potential Chemotherapeutic agents, a new series of 2-anilinobenzimidazol derivatives with CDK activity have been synthesized. The newly synthesized compounds have been assessed for their cytotoxic effects and CDK activity. These presented compounds showed strong inhibition of cell proliferation in various solid cancer cell lines, suggesting a promising approach for treating malignant tumors. Compounds 4 g, 4j, 4 m, and 4q displayed remarkably strong anticancer potencies against HepG2 cells, with IC50 of 7.59, 8.54, 3.56 and 5.88 µM, respectively, compared to the positive control, DOX (IC50 = 4.50 µM). while compound 4 m, and 4q had the highest anticancer activity against HeLa cells, with an IC50 of 6.39 and 9.71 µM, respectively, compared to the positive control DOX (IC50 = 5.57 µM). On the other hand, comparison of IC50 values against MCF-7 cells revealed that compounds 4 g, 4 m, and 4q showed significant anticancer potency with IC50 of 5.08, 2.18 and 8.19 µM, respectively compared to that of the positive control DOX (IC50 = 4.17 µM). Moreover, compound 4 m and 4q were the most potent CDK9 and CDK12 inhibitors. Furthermore, a molecular docking simulation were performed to explore the ability of compounds 4 m to adopt the common binding pattern of CDK9 and CDK12/T1 inhibitors. In silico ADMET results showed that all compounds have favourable drug-like properties since they met Lipinski’s rule of five criteria. Overall, the synthesized anilinopyrimidine derivatives exhibit significant potential as chemotherapeutic agents.
ISSN:1319-0164
2213-7475

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