Zeng De-Ying, Kuang Guo-Tao, Wang Shi-Ke, Peng Wang, Lin Shu-Ling, Zhang Qi, Su Xiao-Xuan, Hu Ming-Hao, Wang Honggen, Tan Jia-Heng, Huang Zhi-Shu, Gu Lian-Quan, Ou Tian-Miao
School of Pharmaceutical Sciences, Sun Yat-sen University , Guangzhou 510006, People's Republic of China.
J Med Chem. 2017 Jul 13;60(13):5407-5423. doi: 10.1021/acs.jmedchem.7b00016. Epub 2017 Jun 16.
The specificity of nucleic acids' binders is crucial for developing this kind of drug, especially for novel G-quadruplexes' binders. Quindoline derivatives have been developed as G-quadruplex stabilizers with good interactive activities. In order to improve the selectivity and binding affinity of quindoline derivatives as c-myc G-quadruplex binding ligands, novel triazole containing benzofuroquinoline derivatives (T-BFQs) were designed and synthesized by using the 1,3-dipolar cycloaddition of a series of alkyne and azide building blocks. The selectivity toward c-myc G-quadruplex DNA of these novel T-BFQs was significantly improved, together with an obvious increase on binding affinity. Further cellular and in vivo experiments indicated that the T-BFQs showed inhibitory activity on tumor cells' proliferation, presumably through the down-regulation of transcription of c-myc gene. Our findings broadened the modification strategies of specific G-quadruplex stabilizers.
核酸结合剂的特异性对于开发这类药物至关重要,尤其是对于新型G-四链体结合剂。喹啉衍生物已被开发为具有良好相互作用活性的G-四链体稳定剂。为了提高喹啉衍生物作为c-myc G-四链体结合配体的选择性和结合亲和力,通过一系列炔烃和叠氮化物构建块的1,3-偶极环加成反应设计并合成了新型含三唑苯并呋喃喹啉衍生物(T-BFQ)。这些新型T-BFQ对c-myc G-四链体DNA的选择性显著提高,同时结合亲和力也明显增加。进一步的细胞和体内实验表明,T-BFQ对肿瘤细胞增殖具有抑制活性,可能是通过下调c-myc基因的转录实现的。我们的研究结果拓宽了特异性G-四链体稳定剂的修饰策略。
