Fragment Optimization of Reversible Binding to the Switch II Pocket on KRAS Leads to a Potent, In Vivo Active KRASG12C Inhibitor

被引:43
作者
Broeker, Joachim [1 ]
Waterson, Alex G. [2 ]
Smethurst, Chris [1 ]
Kessler, Dirk [1 ]
Boettcher, Jark [1 ]
Mayer, Moriz [1 ]
Gmaschitz, Gerhard [1 ]
Phan, Jason [2 ]
Little, Andrew [2 ]
Abbott, Jason R. [2 ,3 ]
Sun, Qi [2 ,3 ]
Gmachl, Michael [1 ]
Rudolph, Dorothea [1 ]
Arnhof, Heribert [1 ]
Rumpel, Klaus [1 ]
Savarese, Fabio [1 ]
Gerstberger, Thomas [1 ]
Mischerikow, Nikolai [1 ]
Treu, Matthias [1 ]
Herdeis, Lorenz [1 ]
Wunberg, Tobias [1 ]
Gollner, Andreas [1 ]
Weinstabl, Harald [1 ]
Mantoulidis, Andreas [1 ]
Kraemer, Oliver [1 ]
McConnell, Darryl B. [1 ]
Fesik, Stephen W. [2 ]
机构
[1] Boehringer Ingelheim RCV GmbH & Co KG, A-1121 Vienna, Austria
[2] Vanderbilt Univ, Dept Biochem, Sch Med, Nashville, TN 37232 USA
[3] AbbVie, 1 North Waukegan Rd, N Chicago, IL 60064 USA
来源
JOURNAL OF MEDICINAL CHEMISTRY | 2022年 / 65卷 / 21期
基金
美国国家卫生研究院;
关键词
SMALL MOLECULES; AMG; 510; K-RAS; DISCOVERY;
D O I
10.1021/acs.jmedchem.2c01120
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Activating mutations in KRAS are the most frequent oncogenic alterations in cancer. The oncogenic hotspot position 12, located at the lip of the switch II pocket, offers a covalent attachment point for KRASG12C inhibitors. To date, KRASG12C inhibitors have been discovered by first covalently binding to the cysteine at position 12 and then optimizing pocket binding. We report on the discovery of the in vivo active KRASG12C inhibitor BI-0474 using a different approach, in which small molecules that bind reversibly to the switch II pocket were identified and then optimized for non-covalent binding using structure-based design. Finally, the Michael acceptor containing warhead was attached. Our approach offers not only an alternative approach to discovering KRASG12C inhibitors but also provides a starting point for the discovery of inhibitors against other oncogenic KRAS mutants.
引用
收藏
页码:14614 / 14629
页数:16
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