| Literature DB >> 34668706 |
Florian Wittlinger1, David E Heppner2, Ciric To3, Marcel Günther1, Bo Hee Shin3, Jaimin K Rana2, Anna M Schmoker2, Tyler S Beyett2, Lena M Berger4,5, Benedict-Tilman Berger4,5, Nicolas Bauer4,5, James D Vasta6, Cesear R Corona6, Matthew B Robers6, Stefan Knapp4,5, Pasi A Jänne3,7, Michael J Eck2, Stefan A Laufer1,8,9.
Abstract
Inhibitors targeting the epidermal growth factor receptor (EGFR) are an effective therapy for patients with non-small cell lung cancer harboring drug-sensitive activating mutations in the EGFR kinase domain. Drug resistance due to treatment-acquired mutations has motivated the development of successive generations of inhibitors that bind in the ATP site. The third-generation agent osimertinib is now a first-line treatment for this disease. Recently, allosteric inhibitors have been developed to overcome drug-resistant mutations that confer a resistance to osimertinib. Here, we present the structure-guided design and synthesis of a mutant-selective lead compound, which consists of a pyridinyl imidazole-fused benzylisoindolinedione scaffold that simultaneously occupies the orthosteric and allosteric sites. The compound potently inhibits enzymatic activity in L858R/T790M/C797S mutant EGFR (4.9 nM), with a significantly lower activity for wild-type EGFR (47 nM). Additionally, this compound achieves modest cetuximab-independent and mutant-selective cellular efficacies on the L858R (1.2 μM) and L858R/T790M (4.4 μM) variants.Entities:
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Year: 2021 PMID: 34668706 PMCID: PMC9255384 DOI: 10.1021/acs.jmedchem.1c00848
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 8.039