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钌(II)的混合配体二亚胺-胡椒醛硫代半卡巴腙配合物的合成与表征:作为抗癌和抗菌剂的生物物理研究及生物学评价

Synthesis and characterization of mixed-ligand diimine-piperonal thiosemicarbazone complexes of ruthenium(II): Biophysical investigations and biological evaluation as anticancer and antibacterial agents.

作者信息

Beckford Floyd A, Thessing Jeffrey, Shaloski Michael, Mbarushimana P Canisius, Brock Alyssa, Didion Jacob, Woods Jason, Gonzalez-Sarrías Antonio, Seeram Navindra P

机构信息

Science Division, Lyon College, Batesville, AR 72501, USA.

出版信息

J Mol Struct. 2011 Apr 19;992(1-3):39-47. doi: 10.1016/j.molstruc.2011.02.029.

Abstract

We have used a novel microwave-assisted method developed in our laboratories to synthesize a series of ruthenium-thiosemicarbazone complexes. The new thiosemicarbazone ligands are derived from benzo[d][1,3]dioxole-5-carbaldehyde (piperonal) and the complexes are formulated as (diimine)(2)Ru(TSC)(2) (where the TSC is the bidentate thiosemicarbazone ligand). The diimine in the complexes is either 2,2'-bipyridine or 1,10-phenanthroline. The complexes have been characterized by spectroscopic means (NMR, IR and UV-Vis) as well as by elemental analysis. We have studied the biophysical characteristics of the complexes by investigating their anti-oxidant ability as well as their ability to disrupt the function of the human topoisomerase II enzyme. The complexes are moderately strong binders of DNA with binding constants of 10(4) M(-1). They are also strong binders of human serum albumin having binding constants on the order of 10(4) M(-1). The complexes show good in vitro anticancer activity against human colon cancer cells, Caco-2 and HCT-116 and indeed show some cytotoxic selectivity for cancer cells. The IC(50) values range from 7 - 159 μM (after 72 h drug incubation). They also have antibacterial activity against Gram-positive strains of pathogenic bacteria with IC(50) values as low as 10 μM; little activity was seen against Gram-negative strains. It has been established that all the compounds are catalytic inhibitors of human topoisomerase II.

摘要

我们采用了在我们实验室开发的一种新型微波辅助方法来合成一系列钌-硫代半卡巴腙配合物。新型硫代半卡巴腙配体衍生自苯并[d][1,3]二氧戊环-5-甲醛(胡椒醛),配合物的化学式为(二亚胺)(2)Ru(TSC)(2)(其中TSC为双齿硫代半卡巴腙配体)。配合物中的二亚胺为2,2'-联吡啶或1,10-菲咯啉。通过光谱手段(核磁共振、红外和紫外可见光谱)以及元素分析对配合物进行了表征。我们通过研究配合物的抗氧化能力以及它们破坏人拓扑异构酶II功能的能力,来研究其生物物理特性。这些配合物是中等强度的DNA结合剂,结合常数为10(4) M(-1)。它们也是人血清白蛋白的强结合剂,结合常数约为10(4) M(-1)。这些配合物对人结肠癌细胞Caco-2和HCT-116显示出良好的体外抗癌活性,并且确实对癌细胞表现出一定的细胞毒性选择性。IC(50)值范围为7 - 159 μM(药物孵育72小时后)。它们对革兰氏阳性病原菌也有抗菌活性,IC(50)值低至10 μM;对革兰氏阴性菌株几乎没有活性。已经确定所有化合物都是人拓扑异构酶II的催化抑制剂。

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