Perin Nataša, Nhili Raja, Cindrić Maja, Bertoša Branimir, Vušak Darko, Martin-Kleiner Irena, Laine William, Karminski-Zamola Grace, Kralj Marijeta, David-Cordonnier Marie-Hélène, Hranjec Marijana
Department of Organic Chemistry, Faculty of Chemical Engineering and Technology, University of Zagreb, Marulićev trg 20, P.O. Box 177, HR-10000 Zagreb, Croatia.
INSERM UMR-S1172, Jean-Pierre Aubert Research Centre (JPARC), Université de Lille, Institut pour la Recherche sur le Cancer de Lille, Place de Verdun, F-59045 Lille cedex, France.
Eur J Med Chem. 2016 Oct 21;122:530-545. doi: 10.1016/j.ejmech.2016.07.007. Epub 2016 Jul 9.
We describe the synthesis, 3D-derived quantitative structure-activity relationship (QSAR), antiproliferative activity and DNA binding properties of a series of 2-amino, 5-amino and 2,5-diamino substituted benzimidazo[1,2-a]quinolines prepared by environmentally friendly uncatalyzed microwave assisted amination. The antiproliferative activities were assessed in vitro against colon, lung and breast carcinoma cell lines; activities ranged from submicromolar to micromolar. The strongest antiproliferative activity was demonstrated by 2-amino-substituted analogues, whereas 5-amino and or 2,5-diamino substituted derivatives resulted in much less activity. Derivatives bearing 4-methyl- or 3,5-dimethyl-1-piperazinyl substituents emerged as the most active. DNA binding properties and the mode of interaction of chosen substituted benzimidazo[1,2-a]quinolines prepared herein were studied using melting temperature studies, a series of spectroscopic studies (UV/Visible, fluorescence, and circular dichroism), and biochemical experiments (topoisomerase I-mediated DNA relaxation and DNase I footprinting experiments). Both compound 36 and its bis-quaternary iodide salt 37 intercalate between adjacent base pairs of the DNA helix while compound 33 presented a very weak topoisomerase I poisoning activity. A 3D-QSAR analysis was performed to identify hydrogen bonding properties, hydrophobicity, molecular flexibility and distribution of hydrophobic regions as these molecular properties had the highest impact on the antiproliferative activity against the three cell lines.
我们描述了通过环境友好的无催化微波辅助胺化反应制备的一系列2-氨基、5-氨基和2,5-二氨基取代的苯并咪唑并[1,2-a]喹啉的合成、三维定量构效关系(QSAR)、抗增殖活性和DNA结合特性。在体外评估了对结肠、肺癌和乳腺癌细胞系的抗增殖活性;活性范围从亚微摩尔到微摩尔。2-氨基取代的类似物表现出最强的抗增殖活性,而5-氨基和/或2,5-二氨基取代的衍生物活性则低得多。带有4-甲基-或3,5-二甲基-1-哌嗪基取代基的衍生物活性最高。使用熔点研究、一系列光谱研究(紫外/可见、荧光和圆二色性)以及生化实验(拓扑异构酶I介导的DNA松弛和DNase I足迹实验)研究了本文制备的选定取代苯并咪唑并[1,2-a]喹啉的DNA结合特性和相互作用模式。化合物36及其双季铵碘盐37都插入到DNA螺旋的相邻碱基对之间,而化合物33表现出非常弱的拓扑异构酶I中毒活性。进行了三维定量构效关系分析,以确定氢键特性、疏水性、分子柔韧性和疏水区域的分布,因为这些分子特性对针对三种细胞系的抗增殖活性影响最大。
