Lv Peng-Cheng, Agama Keli, Marchand Christophe, Pommier Yves, Cushman Mark
Department of Medicinal Chemistry and Molecular Pharmacology, College of Pharmacy, and the Purdue Center for Cancer Research, Purdue University , West Lafayette, Indiana 47907, United States.
J Med Chem. 2014 May 22;57(10):4324-36. doi: 10.1021/jm500294a. Epub 2014 May 6.
Tyrosyl-DNA phosphodiesterase I (TDP1) repairs stalled topoisomerase I (Top1)-DNA covalent complexes and has been proposed to be a promising and attractive target for cancer treatment. Inhibitors of TDP1 could conceivably act synergistically with Top1 inhibitors and thereby potentiate the effects of Top1 poisons. This study describes the successful design and synthesis of 2-position-modified indenoisoquinolines as dual Top1-TDP1 inhibitors using a structure-based drug design approach. Enzyme inhibition studies indicate that indenoisoquinolines modified at the 2-position with three-carbon side chains ending with amino substituents show both promising Top1 and TDP1 inhibitory activity. Molecular modeling of selected target compounds bound to Top1 and TDP1 was used to rationalize the enzyme inhibition results and structure-activity relationship analysis.
酪氨酰-DNA磷酸二酯酶I(TDP1)可修复停滞的拓扑异构酶I(Top1)-DNA共价复合物,并且有人提出它是一个有前景且具吸引力的癌症治疗靶点。TDP1抑制剂可以想象地与Top1抑制剂协同作用,从而增强Top1毒素的效果。本研究描述了使用基于结构的药物设计方法成功设计并合成2-位修饰的茚并异喹啉作为Top1-TDP1双重抑制剂。酶抑制研究表明,在2-位用末端带有氨基取代基的三碳侧链修饰的茚并异喹啉显示出有前景的Top1和TDP1抑制活性。对与Top1和TDP1结合的选定目标化合物进行分子建模,以合理化酶抑制结果并进行构效关系分析。
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