Synthesis, spectroscopic characterization and in vitro cytotoxicities of new organometallic palladium complexes with biologically active β-diketones; Biological evaluation probing of the interaction mechanism with DNA/Protein and molecular docking

化学 插层(化学) 生物活性 滴定法 立体化学 细胞毒性 DNA 结合常数 圆二色性 对接(动物) 核磁共振波谱 体外 结合位点 有机化学 生物化学 医学 护理部
作者
Kazem Karami,Mina Rafiee,Zohreh Mehri Lighvan,Mostafa Zakariazadeh,Ali Yeganeh‐Faal,Seyed‐Alireza Esmaeili,Amir Abbas Momtazi‐Borojeni
出处
期刊:Journal of Molecular Structure [Elsevier]
卷期号:1154: 480-495 被引量:26
标识
DOI:10.1016/j.molstruc.2017.10.059
摘要

[Pd{(C,N)C6H4CH (CH3)NH}(CUR)] (3) and [Pd2{(C,N)C6H4CH(CH3)NH2}2(μ-N3CS2)] (4) [cur = 1,7-bis(4-hydroxy-3-methoxyphenyl)-1,6-heptadiene-3,5-dion] novel organometallic complexes with biologically active ligands have been prepared and characterized via elemental analysis, multinuclear spectroscopic techniques (1H, and 13C NMR and IR) and their biological activities, including antitumoral activity and DNA-protein interactions have been investigated. Fluorescence spectroscopy used to study the interaction of the complexes with BSA have shown the affinity of the complexes for these proteins with relatively high binding constant values and the changed secondary structure of BSA in the presence of the complexes. In the meantime, spectroscopy and competitive titration have been applied to investigate the interaction of complexes with Warfarin and Ibuprofen site markers for sites I and II, respectively, with BSA. The results have suggested that the locations of complexes 3 and 4 are sites II and I, respectively. UV–Vis spectroscopy, emission titration and helix melting methods have been used to study the interaction of these complexes with CT-DNA, indicating that complexes are bound to CT-DNA by intercalation binding mode. In addition, good cytotoxic activity against MCF-7 (human breast cancer) and JURKAT (human leukemia) cell line has been shown by both complexes whereas low cytotoxicity was exerted on normal peripheral blood mononuclear cells.
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