| Literature DB >> 35450359 |
Chunhui Huang1, Christian Fischer1, Michelle R Machacek1, Stephane Bogen2, Tesfaye Biftu2, Xianhai Huang2, Michael H Reutershan1, Ryan Otte1, Qingmei Hong2, Zhicai Wu2, Yang Yu2, Min Park2, Lei Chen2, Purakkattle Biju2, Ian Knemeyer3, Ping Lu3, Christopher J Kochansky3, Michael Brendan Hicks4, Yong Liu4, Roy Helmy4, Xavier Fradera1, Anthony Donofrio1, Josh Close1, Matthew L Maddess1, Catherine White1, David L Sloman1, Nunzio Sciammetta1, Jun Lu3, Craig Gibeau1, Vladimir Simov1, Hongjun Zhang1, Peter Fuller1, David Witter1.
Abstract
Mutant isocitrate dehydrogenase 1 (IDH1) has been identified as an attractive oncology target for which >70% of grade II and III gliomas and ∼10% of acute myeloid leukemia (AML) harbor somatic IDH1 mutations. These mutations confer a neomorphic gain of function, leading to the production of the oncometabolite (R)-2-hydroxyglutarate (2-HG). We identified and developed a potent, selective, and orally bioavailable brain-penetrant tricyclic diazepine scaffold that inhibits mutant IDH1. During the course of in vitro metabolism studies, GSH-adduct metabolites were observed. The hypothesis for GSH-adduct formation was driven by the electron-rich nature of the tricyclic core. Herein, we describe our efforts to reduce the electron-rich nature of the core. Ultimately, a strategy focused on core modifications to block metabolic hot spots coupled with substitution pattern changes (C8 N → C linked) led to the identification of new tricyclic analogues with minimal GSH-adduct formation across species while maintaining an overall balanced profile.Entities:
Year: 2022 PMID: 35450359 PMCID: PMC9014435 DOI: 10.1021/acsmedchemlett.2c00089
Source DB: PubMed Journal: ACS Med Chem Lett ISSN: 1948-5875 Impact factor: 4.345