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Mohammad Satari keykeleh

Mohammad Satari keykeleh

Academic rank: Assistant Professor
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Education: PhD.
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Faculty: science
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Research

Title
In vitro cytotoxicity evaluation of organotin (IV) complexes derived from bisphosphoramide ligand: DNA binding and molecular docking studies
Type
JournalPaper
Keywords
Keywords: Organotin(IV) complexes Bisphosphoramide ligands Molecular docking Cytotoxicity DNA binding Anticancer activity
Year
2023
Journal journal of molecular liquids
DOI
Researchers Mohammad Satari keykeleh

Abstract

Considering the valuable position of organotins and the biotic role of phosphorus compounds in biological processes, in this research work, we investigated and introduced a new class of anticancer candidates based on organotin(IV) complexes derived from bisphosphoramide ligands. Four selected complexes were prepared from the reaction of SnMe2Cl2 (C1), SnBu3Cl (C2), SnPh2Cl2 (C3), and SnPh3Cl (C4) metal salts with piperazine-1,4- diylbis(diphenylphosphine oxide) ligand (LP). The newly synthesized complexes were characterized using spectroscopic techniques. Single crystal of C1 structure was determined by X-ray crystallography. Binding potentials of compounds to DNA were also explored using electron absorption titration and competitive fluorescence quenching techniques, which indicated that complexes and CT-DNA strongly interacted. Cytotoxicity assay of compounds against triple-negative human breast cancer (MDA-MB-231) cells proved that three complexes C2, C3, and C4 had a very considerable impact on the reduced viability of cancer cells and among them, C4 revealed the maximum anticancer activity (IC50 = 0.35 ± 1.18 μg/mL, 0.28 μM) in comparison to reference cisplatin drug (IC50 = 19 μM). Furthermore, the analysis and comparison of the orientations and reactive sites of the compounds using molecular docking simulation, pharmacophore, and NCI studies further confirmed the significant effects of the type and number of aryl and alkyl substituents on the biological activities.