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چکیده
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Despite significant progress in cancer treatment, cancer remains a major focus of research due to
medication resistance and side effects. In this study, bioactive adamantane-containing dihydropyrimidine
(DHPM) derivatives were synthesized through the multi-component Biginelli reaction of N-(adamant-1-
yl)acetoacetamide, benzaldehyde derivatives, and thiourea in the presence of trifluoroacetic acid (TFA,
2 mol%) as catalyst under solvent free conditions. This method provides an effective and significantly
improved modification of the original Biginelli reaction in terms of yield and reaction time. The
synthesized DHPM derivatives were subjected to cytotoxicity screening against the A-549 human nonsmall
cell lung cancer (NSCLC) cell line to evaluate their effects on cell growth inhibition. MTT
cytotoxicity assay was used to determine IC50 values. Among the target analogs, IIb, IIj, IId, and IIg
demonstrated the best activity with IC50 values of 1.03, 8.36, 10.38, and 16.04 mg mL−1, respectively.
Additionally, we assessed the possible mechanisms for cell growth inhibition and induction of apoptotic
cell death using the DAPI and Annexin V-FITC staining. The average percentages of apoptotic cells were
21.35%, 28.35%, 32.73, and 43.33% for IIg, IId, IIj, and IIb treatment groups, respectively. These results
suggest that the synthesized adamantane-containing dihydropyrimidines can be considered as
encouraging molecules for further drug development as anticancer agents.
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