Two series of cyanopyrimidine hybrids were synthesized bearing either benzo[]imidazole, benzo[]oxazole, benzo[]thiazole, and benzo[]thiophene derivatives via methylene amino linker - (Formula A) or various sulphonamide phenyl moieties - (Formula B) at the C-2 position. All compounds' cyclooxygenase COX-2 inhibitory activities were evaluated, and all synthesized compounds demonstrated potent activity at minimal concentrations, with IC values in the submicromolar range. Compounds , , and were discovered to be the most active pyrimidine derivatives, with the highest COX-2 percent inhibition and IC values being nearly equal to Celecoxib and approximately 4.7-, 9.3-, and 10.5-fold higher than Nimesulide. Furthermore, the pyrimidine derivatives , , and demonstrated anticancer activity comparable to or better than doxorubicin against four cell lines, i.e., MCF-7, A549, A498, and HepG2, with IC values in nanomolar in addition to low cytotoxicity on the normal W38-I cell line. The effect of compound on cell cycle progression and apoptosis induction was investigated, and it was found that compound could seize cell growth at the sub-G1 and G2/M phases, as well as increase the proportion of early and late apoptotic rates in MCF-7 cells by nearly 13- and 60-fold, respectively. Moreover, in silico studies for compounds , , and revealed promising findings, such as strong GIT absorption, absence of BBB permeability, nil-to-low drug-drug interactions, good oral bioavailability, and optimal physicochemical properties, indicating their potential as promising therapeutic candidates.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9658812PMC
http://dx.doi.org/10.3390/molecules27217485DOI Listing

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