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New Combretastatin Analogs as Anticancer Agents: Design, Synthesis, Microtubules Polymerization Inhibition, and Molecular Docking Studies

Shaker A. Abdul Hussein, Ammar A. Razzak Mahmood, Lubna H. Tahtamouni, Asim A. Balakit, Yahya Saad Yaseen, Rehab A. M. Al-Hasani

2023Chemistry & Biodiversity12 citationsDOIOpen Access PDF

Abstract

Abstract A new series of 4‐(4‐methoxyphenyl)‐5‐(3,4,5‐trimethoxyphenyl)‐4 H‐ 1,2,4‐triazole‐3‐thiol derivatives were synthesized as analogs for the anticancer drug combretastatin A‐4 ( CA‐4 ) and characterized using FT‐IR, 1 H‐NMR, 13 CNMR, and HR‐MS techniques. The new CA‐4 analogs were designed to meet the structural requirements of the highest expected anticancer activity of CA‐4 analogs by maintaining ring A 3,4,5‐trimethoxyphenyl moiety, and at the same time varying the substituents effect of the triazole moiety (ring B ). In silico analysis indicated that compound 3 has higher total energy and dipole moment than colchicine and the other analogs, and it has excellent distribution of electron density and is more stable, resulting in an increased binding affinity during tubulin inhibition. Additionally, compound 3 was found to interact with three apoptotic markers, namely p53, Bcl‐2, and caspase 3. Compound 3 showed strong similarity to colchicine , and it has excellent pharmacokinetics properties and a good dynamic profile. The in vitro anti‐proliferation studies showed that compound 3 is the most cytotoxic CA‐4 analog against cancer cells (IC 50 of 6.35 μM against Hep G2 hepatocarcinoma cells), and based on its selectivity index (4.7), compound 3 is a cancer cytotoxic‐selective agent. As expected and similar to colchicine , compound 3 ‐treated Hep G2 hepatocarcinoma cells were arrested at the G2/M phase resulting in induction of apoptosis. Compound 3 tubulin polymerization IC 50 (9.50 μM) and effect on V max of tubulin polymerization was comparable to that of colchicine (5.49 μM). Taken together, the findings of the current study suggest that compound 3 , through its binding to the colchicine‐binding site at β‐tubulin, is a promising microtubule‐disrupting agent with excellent potential to be used as cancer therapeutic agent.

Topics & Concepts

CombretastatinChemistryTubulinStereochemistryMoietyDocking (animal)MicrotubuleMedicineBiologyCell biologyNursingSynthesis and biological activityClick Chemistry and ApplicationsSynthesis and Characterization of Heterocyclic Compounds
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