电合成
化学
组合化学
脚手架
拓扑异构酶
药物发现
纳米技术
计算机科学
电化学
生物化学
电极
材料科学
DNA
物理化学
数据库
作者
Yue‐Xi Chen,Shanchao Wu,Xiang Shen,Dongfang Xu,Qian Wang,Su‐Hui Ji,Huajian Zhu,Ge Wu,Chunquan Sheng,Yun‐Rui Cai
标识
DOI:10.1002/chem.202401400
摘要
Coumestan represents a biologically relevant structural motif distributed in a number of natural products, and the rapid construction of related derivatives as well as the characterization of targets would accelerate lead compound discovery in medicinal chemistry. In this work, a general and scalable approach to 8,9-dihydroxycoumestans via two-electrode constant current electrolysis was developed. The application of a two-phase (aqueous/organic) system plays a crucial role for success, protecting the sensitive o-benzoquinone intermediates from over-oxidation. Based on the structurally diverse products, a primary SAR study on coumestan scaffold was completed, and compound 3 r exhibited potent antiproliferative activities and a robust topoisomerase I (Top1) inhibitory activity. Further mechanism studies demonstrates that compound 3 r was a novel Top1 poison, which might open an avenue for the development of Top1-targeted antitumor agent.
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