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首页> 外文期刊>New Journal of Chemistry >A water-soluble Pd(II) complex with a terpyridine ligand: experimental and molecular modeling studies of the interaction with DNA and BSA; and in vitro cytotoxicity investigations against five human cancer cell lines
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A water-soluble Pd(II) complex with a terpyridine ligand: experimental and molecular modeling studies of the interaction with DNA and BSA; and in vitro cytotoxicity investigations against five human cancer cell lines

机译:具有吡啶吡啶配体的水溶性Pd(II)配合物:与DNA和BSA相互作用的实验和分子模型研究;和对五种人类癌细胞系的体外细胞毒性研究

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摘要

A new Pd(II) complex, [Pd(4-OHPh-tpy)Cl]Cl, with a ligand that is a terpyridine derivative, (4 '-(4-hydroxyphenyl)-2,2 ',6 ',2 ''-terpyridine (4-OHPh-tpy)), was prepared and fully characterized. The single crystal structures of 4-OHPh-tpy and its Pd(II) complex were determined by X- ray crystallography. The in vitro studies (UV-Vis spectroscopy, circular dichroism (CD), rheometry, and gel electrophoresis) show that the Pd(II) complex interacts with calf- thymus DNA (CT-DNA) via a combination of covalent, intercalation, and hydrogen bonding interactions, whereas the free 4-OHPh-tpy ligand interacts with DNA mainly through intercalation. The Pd(II) complex cleaves the supercoiled double- stranded DNA under physiological conditions without the need to add an external reductant. The microenvironment and the secondary structure of BSA were also changed in the presence of both the free ligand and the Pd(II) complex. The Pd(II) complex was remarkable in exhibiting cleavage of the BSA at micromolar concentrations and short incubation times at physiological pH and temperature. The anti- cancer effects of the free ligand and the Pd(II) complex were tested in vitro against five human tumor cell lines, including the human breast cancer cell line (MCF-7), lung adenocarcinoma cells (A-549), an erythroleukemic cell line (K562), a colorectal adenocarcinoma cell line (HT-29), and hepatocellular carcinoma (Hep-G2) cells. The Pd(II) complex showed the IC50 values less than those of cisplatin against the MCF- 7, A- 549, K562, and HT- 29 cancer cell lines. Finally, the binding of the Pd(II) complex and 4-OHPh-tpy to BSA and DNA was modeled by molecular docking and molecular dynamic simulation methods.
机译:一种新的Pd(II)络合物[Pd(4-OHPh-tpy)Cl] Cl,其配体为三联吡啶衍生物,(4'-(4-羟基苯基)-2,2',6',2'制备并完全表征了β-联吡啶(4-OHPh-tpy)。通过X射线晶体学测定4-OHPh-tpy及其Pd(II)配合物的单晶结构。体外研究(UV-Vis光谱,圆二色性(CD),流变学和凝胶电泳)表明,Pd(II)配合物通过共价,嵌入和三价结合而与小胸腺DNA(CT-DNA)相互作用。氢键相互作用,而游离的4-OHPh-tpy配体主要通过嵌入与DNA相互作用。 Pd(II)络合物可在生理条件下切割超螺旋双链DNA,而无需添加外部还原剂。在存在游离配体和Pd(II)复合物的情况下,BSA的微环境和二级结构也发生了变化。 Pd(II)复合物在微摩尔浓度下表现出BSA的裂解,在生理pH和温度下的孵育时间短,因此表现出色。在体外测试了游离配体和Pd(II)配合物对五种人类肿瘤细胞系的抗癌作用,其中包括人类乳腺癌细胞系(MCF-7),肺腺癌细胞(A-549),红白血病细胞系(K562),结肠直肠腺癌细胞系(HT-29)和肝细胞癌(Hep-G2)细胞。 Pd(II)复合物对MCF-7,A-549,K562和HT-29癌细胞系的IC50值低于顺铂。最后,通过分子对接和分子动力学模拟方法对Pd(II)复合物和4-OHPh-tpy与BSA和DNA的结合进行了建模。

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