| Literature DB >> 31689114 |
Harald Engelhardt1, Dietrich Böse1, Mark Petronczki1, Dirk Scharn1, Gerd Bader1, Anke Baum1, Andreas Bergner1, Eugene Chong2, Sandra Döbel1, Georg Egger1, Christian Engelhardt1, Peter Ettmayer1, Julian E Fuchs1, Thomas Gerstberger1, Nina Gonnella2, Andreas Grimm1, Elisabeth Grondal1, Nizar Haddad2, Barbara Hopfgartner1, Roland Kousek1, Mariusz Krawiec2, Monika Kriz1, Lyne Lamarre1, Joyce Leung2, Moriz Mayer1, Nitinchandra D Patel2, Biljana Peric Simov1, Jonathan T Reeves2, Renate Schnitzer1, Andreas Schrenk1, Bernadette Sharps1, Flavio Solca1, Heinz Stadtmüller1, Zhulin Tan2, Tobias Wunberg1, Andreas Zoephel1, Darryl B McConnell1.
Abstract
The epidermal growth factor receptor (EGFR), when carrying an activating mutation like del19 or L858R, acts as an oncogenic driver in a subset of lung tumors. While tumor responses to tyrosine kinase inhibitors (TKIs) are accompanied by marked tumor shrinkage, the response is usually not durable. Most patients relapse within two years of therapy often due to acquisition of an additional mutation in EGFR kinase domain that confers resistance to TKIs. Crucially, oncogenic EGFR harboring both resistance mutations, T790M and C797S, can no longer be inhibited by currently approved EGFR TKIs. Here, we describe the discovery of BI-4020, which is a noncovalent, wild-type EGFR sparing, macrocyclic TKI. BI-4020 potently inhibits the above-described EGFR variants and induces tumor regressions in a cross-resistant EGFRdel19 T790M C797S xenograft model. Key was the identification of a highly selective but moderately potent benzimidazole followed by complete rigidification of the molecule through macrocyclization.Entities:
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Year: 2019 PMID: 31689114 DOI: 10.1021/acs.jmedchem.9b01169
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446