Synthesis, Antiproliferative Activity and In Silico Studies of Chalcones Derived From 4-(Imidazole-1-yl)Acetophenone

Bedriye Seda KURŞUN AKTAR, Abdulraheem Mustafa Alkarabash, A. ŞAHİN YAĞLIOĞLU, E. E. Oruç-Emre
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Abstract

In this study, the synthesis of chalcone compounds (1-11) derived from 4-(imidazol-1-yl)acetophenone and the structure determination of these compounds by various spectroscopic methods were carried out. The anticancer activities of compounds 1-11 were examined against HeLa and PC-3 cancer cells at four different concentrations (100, 50, 25, and 5 µM) using the BrdU ELISA assay. It was determined that all molecules except compounds 1 and 6 in HeLa cancer cells and compounds 2 and 8 against PC-3 cancer cells were more active against HeLa and PC-3 than the standard drug 5-fluorouracil (5-FU). The best activity against PC-3 cancer cells was compound 4 (IC50: 1.39±0.00 µM). In addition, compound 11 (IC50: 1.58±0.01 µM) was found to have the highest activity against HeLa cancer cells. Compound 4 against PC-3 cancer cell and compound 11 against HeLa cancer cell displayed cell selective activity. The ADME properties and drug similarities of the molecules 1-11 using the SwissADME software were investigated. According to these properties, compounds 1-11 were found to obey Lipinski rules.
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4-(咪唑-1-基)苯乙酮衍生查尔酮的合成、抗增殖活性及硅研究
本研究合成了由4-(咪唑-1-基)苯乙酮衍生的查尔酮类化合物(1-11),并利用各种光谱方法对其结构进行了测定。采用BrdU ELISA法检测化合物1-11在不同浓度(100、50、25和5µM)下对HeLa和PC-3癌细胞的抗癌活性。结果表明,除HeLa癌细胞中的化合物1、6和PC-3癌细胞中的化合物2、8外,其他分子对HeLa和PC-3的活性均高于标准药物5-氟尿嘧啶(5-FU)。化合物4对PC-3癌细胞的抑制活性最高(IC50: 1.39±0.00µM)。化合物11 (IC50: 1.58±0.01µM)的抗HeLa癌细胞活性最高。化合物4对PC-3癌细胞和化合物11对HeLa癌细胞表现出细胞选择性活性。利用SwissADME软件对分子1-11的ADME性质和药物相似性进行了研究。根据这些性质,化合物1-11符合利平斯基规则。
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