Design, synthesis, preliminary pharmacological evaluation, molecular docking and ADME studies of some new pyrazoline, isoxazoline and pyrimidine derivatives bearing nabumetone moiety targeting cyclooxygenase enzyme

Yousif, Omar A.; Mahdi, Monther F.; Raauf, Ayad M.R.

doi:10.22317/jcms.v5i1.521

Cited by 11 publications

(1 citation statement)

References 35 publications

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“…Furthermore, a significant amount of research has shown that heterocycles based pyrazole show promising activity against cancer cell lines, including A549 human lung adenocarcinoma and liver cancer cell lines (13)(14)(15) . This pharmacologically-interesting heterocyclic system have been synthesized from the reaction of α,β-unsaturated ketones (chalcone) (1) that have a wide range of pharmacological activities, including antioxidant , anti-tumor , antibacterial , antihistaminic , antifungal, anticancer, antiobesity, anti-inflammatory, anti-spasmodic, anti-malarial, anti-protozoal and cytotoxic properties (16) with benzohydrazide derivatives .…”

Section: Introductionmentioning

confidence: 99%

Molecular docking , Synthesis and ADME Studies of New Pyrazoline Derivatives as Potential Anticancer Agents.

2021

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Cancer is a significant worldwide public health issue. The adverse effects of anticancer chemotherapies still compromise the quality of life of patients. To identify new potential targeted anticancer agents, a series of pyrazoline derivatives were synthesized and evaluated for anticancer effects on A549 (human lung adenocarcenoma cell line). In silico evaluation methods were done before synthesis through molecular docking via genetic optimization for ligand docking (GOLD) Suite software with EGFR tyrosine kinase and exhibited significant tyrosine kinase inhibition activities compared with Erlotinb as a reference drug due to their hydrogen bonding and short contact interaction with key amino acids and these results are compatible with the experimental findings. The new derivatives were synthesized by incorporating pyrazoline pharmacophore into nabumetone moiety as a starting molecule and the chalcone derivatives as intermediate products. The compounds structure were confirmed by 1 H-NMR, some physicochemical properties and infrared spectroscopy. An in vitro assay demonstrated that the final compounds (P1, P2, P3 and P4) exerted potent to moderate cytotoxic activity in the micromolar range with an IC50 values (15.409µM, 7.24µM, 27.05µM, 22.45µM) respectively when compared with Erlotinib (IC50 =25.23µM) while (P5&P6) show weak activity. Pharmacokinetic and physicochemical properties of the final compounds predicted by using ADME evaluations. The results showed all the synthesized compounds have high oral bioavailability and good GI absorption.

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