Chiral heterobimetallic complexes targeting human DNA-topoisomerase Iα

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Abstract

The chiral monometallic CuII (1) and ZnII (2) and heterobimetallic CuII-SnIV and ZnII-Sn IV complexes with tridentate chiral Schiff base -ONO-ligand in the presence of nitrogen donor heterocyclic ligand imidazole; were prepared and characterized by various physico-chemical and spectroscopic methods. Preliminary complex-DNA interaction studies employing optical methods revealed that 3 displayed a higher propensity towards the drug target DNA double helix and recommended predominantly an electrostatic mode of interaction as well as a groove binding affinity of the complex with CT-DNA. This was quantified by Kb and KSV values of complexes 1-4, which demonstrated a multifold increase in complex 3 binding to CT DNA and clearly demonstrates its potency to act as a chemotherapeutic agent. Furthermore, the gel electrophoretic patterns of supercoiled pBR322 DNA with varying concentrations of complex 3 exhibits the ability to cleave DNA and follow a freely diffusible radical mechanism. The antiproliferative effects of complex 3 on human hepatoma cancer cells (Huh7) was investigated. Human Topo I inhibition assay by complex 3 was performed and results confirmed significantly good activity at lower concentrations than some of the classical Topo I inhibitors. Additionally, complex 3 was investigated for the expression of MMP-2 and TGF-β by real time PCR. The cellular uptake of complex 3 by HeLa cells was studied by confocal microscopy. © 2013 The Royal Society of Chemistry.

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Tabassum, S., Asim, A., Khan, R. A., Hussain, Z., Srivastav, S., Srikrishna, S., & Arjmand, F. (2013). Chiral heterobimetallic complexes targeting human DNA-topoisomerase Iα. Dalton Transactions, 42(48), 16749–16761. https://doi.org/10.1039/c3dt51209f

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