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Design synthesis and biological evaluation of arylcinnamide hybrid derivatives as novel anticancer agents

机译:芳基肉桂酰胺杂化衍生物作为新型抗癌药的设计合成及生物学评价

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摘要

The combination of two pharmacophores into a single molecule represents one of the methods that can be adopted for the synthesis of new anticancer molecules. A series of novel antiproliferative agents designed by a pharmacophore hybridization approach, combining the arylcinnamide skeleton and an α-bromoacryloyl moiety, was synthesized and evaluated for its antiproliferative activity against a panel of seven human cancer cell lines. In addition, the new derivatives were also active on multidrug-resistant cell lines over-expressing P-glycoprotein. The biological effects of various substituents on the N-phenyl ring of the benzamide portion were also described. In order to study the possible mechanism of action, we observed that >4p slightly increased the Reactive Oxygen Species (ROS) production in HeLa cells, but, more importantly, a remarkable decrease of intracellular reduced glutathione content was detected in treated cells compared with controls. These results were confirmed by the observation that only thiol-containing antioxidants were able to significantly protect the cells from induced cell death. Altogether our results indicate that the new derivatives are endowed with good anticancer activity in vitro, and their properties may result in the development of new cancer therapeutic strategies.
机译:将两个药效基团组合成单个分子代表了可用于合成新抗癌分子的方法之一。合成了一系列通过药效基团杂交方法设计的新型抗增殖剂,结合了芳基肉桂酰胺骨架和α-溴丙烯酰基部分,并评估了其对一组七种人类癌细胞系的抗增殖活性。此外,新的衍生物还对过表达P-糖蛋白的多药耐药细胞系具有活性。还描述了各种取代基对苯甲酰胺部分的N-苯环的生物学影响。为了研究可能的作用机理,我们观察到> 4p 略微增加了HeLa细胞中的活性氧(ROS)产生,但更重要的是,检测到细胞内减少的谷胱甘肽含量明显降低与对照组相比通过观察证实了这些结果,只有含硫醇的抗氧化剂才能显着保护细胞免受诱导的细胞死亡。总的来说,我们的结果表明新衍生物在体外具有良好的抗癌活性,其性质可能导致新的癌症治疗策略的发展。

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