Invitro cytotoxicity and DNA interaction studies of nickel(II) mefenamato compounds with substituted α-diimines
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Date
2025
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Elsevier
Abstract
Two bioactive nickel(II) compounds of mefenamic acid (Hmef) with substituted α-diimines as co-ligands have been characterised using various spectroscopic methods and evaluated for cytotoxicity, DNA interaction and antioxidant studies, molecular docking and dynamics studies. Single crystal structures of [Ni(Mef-O)2(etobpy)(H2O)] 1 and [Ni(Mef-O)2(dmbpy)(H2O)(DMF)] 2, (etobpy = 4,4′-diethoxy 2,2′-bipyridine, dbmbpy = 4,4′-dimethyl-2,2′-bipyridine and DMF = N, N′-dimethylformamide) have been determined using single crystal X-ray diffraction technique. The mefenamato ligand adopts two types of coordination modes (mono- and bidentate) in 1, while in compound 2 both mef ligands display monodentate behaviour. The Ni(II) ion in both compounds shows a distorted octahedral geometry binding to two N and four O atoms. The cytotoxicity results revealed the activity of 1 and 2 against cancerous HepG2 in a dose-dependent manner. % DPPH free radical scavenging activity of 1 and 2 when performed, they exhibited IC50 values of 17.02±0.85 μM and 19.89±0.73 μM respectively, depicting their antioxidant nature. DNA binding properties of 1 and 2 were assessed by UV absorption spectroscopy, which suggested an intercalating binding between the complexes and the DNA. Both complexes act as potential agents towards DNA cleavage with the dose-dependent rise of Form II and III DNA. Further, Their interactions with DNA were studied using molecular docking and molecular dynamics simulations. Both 1 and 2 are intercalating in the major groove of DNA fragment, destabilizing the double helix strand during simulation, proving as potential candidates for cytotoxicity.
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NATURAL SCIENCES::Chemistry
Citation
Journal of Molecular Structure Volume. 1332; 2025; 141694 pp.