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Journal of Coordination Chemistry Volume 76, 2023 - Issue 16-24
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Research Article

N’-Ferrocenylmethyl-N’-phenylbenzohydrazide as a potential DNA binding compound: a combined experimental and computational study

Mouada Hananea Department of Process Engineering, Institute of science University Center of Tipaza, Tipaza, AlgeriaCorrespondence[email protected]
,
Touhami Lanezb Department of Chemistry, University of El Oued, El Oued, Algeria;c VTRS Laboratory, El Oued, Algeria
,
Imran Zafard Department of Bioinformatics, Virtual University, Punjab, Pakistan
,
Muhammad Sher Afghane Department of ENT, DHQ Teaching Hospital Faisalabad, Faisalabad, Pakistan
&
Nadjiba Zeghebc VTRS Laboratory, El Oued, Algeria
Pages 1984-1998 | Received 09 Jun 2023, Accepted 28 Aug 2023, Published online: 31 Oct 2023
 
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Abstract

Due to increased lipophilicity, stability, and decreased cytotoxicity in biological systems, ferrocene derivatives are promising building blocks for therapeutic agents. This manuscript reports the binding of N’-ferrocenylmethyl-N’-phenylbenzohydrazide (FhD) with deoxyribonucleic acid (DNA) studied by absorption spectroscopy and cyclic voltammetry. Binding constants and binding free energies for the FhD-DNA complex were measured using these two methods as 5100 M−1, 6109 M−1 and −21.2 kJ/mol, −21.6 kJ/mol, respectively. DFT calculations were also performed and revealed important physical characteristics of the FhD compound. Subsequently, the system was explored by computational molecular docking, confirming a non-covalent mode of binding via minor groove with a binding energy of −25.5 kJ/mol. Furthermore, molecular dynamics of the docked complex of FhD with DNA were carried out for 100 ns followed by MM-GBSA to have a deep understanding of the complex’s dynamic behavior in physiological systems, and to determine the Gibbs free energy which was −14.31 Kcal/mol over a 100 ns window. The results show important antitumor potential of FhD due to its spontaneous non-covalent interaction with DNA and the efficient binding stability of the FhD-DNA complex in a physiological system.

Acknowledgements

The authors are grateful to the Algerian Ministry of Higher Education and Scientific Research for financial support (project code: B00L01UN390120150001) and wish to express their thanks to Mr. Ali Tliba from Laboratory of Valorization and Technology of Saharan Resources, University of El Oued (VTRS) and to his staff for their assistance.

Disclosure statement

The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.

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