首页> 外文期刊>Dalton transactions: An international journal of inorganic chemistry >Experimental and theoretical investigations of cyclometalated ruthenium(ii) complex containing CCC-pincer and anti-inflammatory drugs as ligands: synthesis, characterization, inhibition of cyclooxygenase and in vitro cytotoxicity activities in various cancer cell lines
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Experimental and theoretical investigations of cyclometalated ruthenium(ii) complex containing CCC-pincer and anti-inflammatory drugs as ligands: synthesis, characterization, inhibition of cyclooxygenase and in vitro cytotoxicity activities in various cancer cell lines

机译:含CCC-钳子和抗炎药作为配体的实验和理论研究作为配体:合成,表征,环氧氧酶的抑制和各种癌细胞系中的体外细胞毒性活性

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摘要

The new cyclometalated ruthenium(ii) complex, [Ru(CCC-Nap)(Ibu)(PTA)] was designed and synthesized using ibuprofen (Ibu), 1,3,5-triaza-7-phosphaadamantane (PTA) and CCC-pincer containing naproxen moiety (CCC-Nap) as ligands. The compounds were fully characterized by elemental analysis, FT-IR, multinuclear (H-1, C-13, and P-31) NMR spectroscopy, and electrospray ionization mass spectrometry. The cytotoxicity of the newly synthesized Ru(ii) complex was found to be low, and the complex was about twice as active as cisplatin with IC50 values in the range of 0.9-1.32 M for both MCF-7 and MDA-MB-231 cell lines. Cyclooxygenase (COX) inhibition studies revealed that the Ru(ii) complex displayed strong interactions with COX-2, about 16 and 5 times more than free Ibu and CCC-Nap ligands, respectively. The Ru(ii) complex improved the production of reactive oxygen species (ROS) by 10.7 fold compared to the control (H2O2 as a positive control) in MCF-7 cells. Quantum chemical calculations gave more insights into the geometry and electronic properties of the novel Ru(ii) complex, while molecular docking provided theoretical information on the interactions of Ru(ii) complex with human cyclooxygenase-2 (COX-2) and the results were compared with those of the interactions of the free ligands with COX-2.
机译:使用布洛芬(IBU),1,3,5-Triaza-7-磷AdaMantane(PTA)和CCC-设计和合成了新的环状钌(II)复合物,[Ru(CCC-NAP)(IBU)(IBU)(PTA)]设计和合成含有萘普克克伦部分(CCC-NAP)作为配体的钳子。通过元素分析,FT-IR,多核(H-1,C-13和P-31)NMR光谱和电喷雾电离质谱法完全表征化合物。发现新合成的Ru(II)复合物的细胞毒性为低,并且该复合物在MCF-7和MDA-MB-231细胞的范围内为0.9-1.32μm的IC50值,该复合物是连同铂的两倍。线条。环加氧酶(COX)抑制研究表明,Ru(II)复合物分别显示出与Frea IBU和CCC-NaP配体的大约16和5倍的强烈相互作用。与MCF-7细胞中的对照(H 2 O 2为阳性对照)相比,Ru(II)复合物改善了活性氧物质(ROS)的产生10.7倍。量子化学计算对新型ru(ii)复合物的几何和电子性质进行了更多的见解,而分子对接提供了关于ru(ii)复合物与人环氧基酶-2(Cox-2)的相互作用的理论信息,结果是与具有COX-2的自由配体的相互作用相比。

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