Synthesis and In-Silico Prediction of Pyrimidine Analogues for Anticancer and Antihistaminic Potential
DOI:
https://doi.org/10.64149/J.Carcinog.24.2s.886-893Keywords:
pyrimidine, Biginelli reaction, antihistamine, thymidylate synthase, CDK2, H1 receptor, docking, MM-GBSA, QSAR, ADMETAbstract
Pyrimidines are privileged scaffolds across oncology and allergy therapeutics. We designed and synthesized two focused libraries of pyrimidine analogues—(A) 4,6-disubstituted dihydropyrimidinones (DHPMs) via a Biginelli strategy (n = 16) targeting thymidylate synthase (TS) and cyclin-dependent kinase 2 (CDK2), and (B) 2-anilino-4-(alkoxy)-pyrimidines bearing a distal tertiary amine (n = 12) targeting the human histamine H1 receptor (H1R). In-silico docking suggested sub-micromolar binding modes for lead A-07 (predicted ΔGbind −10.1 kcal/mol to TS; −9.2 kcal/mol to CDK2) and B-05 (−10.3 kcal/mol to H1R). MM-GBSA rescoring corroborated rank ordering. Drug-likeness and ADMET predictions indicated oral bioavailability for 22/28 molecules (Lipinski compliant; low hERG liability) with acceptable metabolic stability. A 2D-QSAR (training n = 20; test n = 8) explained docking-derived pKd with r² = 0.81, Q²_LOO = 0.73, RMSEtest = 0.41. This work presents tractable syntheses and computational evidence prioritizing pyrimidine analogues for dual therapeutic exploration in oncology and antihistamine discovery.
