Development of Novel Dual Binders as Potent, Selective, and Orally Bioavailable Tankyrase Inhibitors
详细信息 查看全文
- 作者:Zihao Hua ; Howard Bregman ; John L. Buchanan ; Nagasree Chakka ; Angel Guzman-Perez ; Hakan Gunaydin ; Xin Huang ; Yan Gu ; Virginia Berry ; Jingzhou Liu ; Yohannes Teffera ; Liyue Huang ; Bryan Egge ; Renee Emkey ; Erin L. Mullady ; Steve Schneider ; Paul S. Andrews ; Lisa Acquaviva ; Jennifer Dovey ; Ankita Mishra ; John Newcomb ; Douglas Saffran ; Randy Serafino ; Craig A. Strathdee ; Susan M. Turci ; Mary Stanton ; Cindy Wilson ; Erin F. DiMauro
- 刊名:Journal of Medicinal Chemistry
- 出版年:2013
- 出版时间:December 27, 2013
- 年:2013
- 卷:56
- 期:24
- 页码:10003-10015
- 全文大小:628K
- ISSN:1520-4804
文摘
Tankyrases (TNKS1 and TNKS2) are proteins in the poly ADP-ribose polymerase (PARP) family. They have been shown to directly bind to axin proteins, which negatively regulate the Wnt pathway by promoting 尾-catenin degradation. Inhibition of tankyrases may offer a novel approach to the treatment of APC-mutant colorectal cancer. Hit compound 8 was identified as an inhibitor of tankyrases through a combination of substructure searching of the Amgen compound collection based on a minimal binding pharmacophore hypothesis and high-throughput screening. Herein we report the structure- and property-based optimization of compound 8 leading to the identification of more potent and selective tankyrase inhibitors 22 and 49 with improved pharmacokinetic properties in rodents, which are well suited as tool compounds for further in vivo validation studies.