| Literature DB >> 35883003 |
Birgit Wilding1, Dirk Scharn2, Dietrich Böse2, Anke Baum2, Valeria Santoro2, Paolo Chetta2, Renate Schnitzer2, Dana A Botesteanu2, Christoph Reiser2, Stefan Kornigg2, Petr Knesl2, Alexandra Hörmann2, Anna Köferle2, Maja Corcokovic2, Simone Lieb2, Guido Scholz2, Jens Bruchhaus2, Markus Spina2, Josef Balla2, Biljana Peric-Simov2, Jasmin Zimmer2, Sophie Mitzner2, Thomas N Fett2, Alexandra Beran2, Lyne Lamarre2, Thomas Gerstberger2, Daniel Gerlach2, Markus Bauer2, Andreas Bergner2, Andreas Schlattl2, Gerd Bader2, Matthias Treu2, Harald Engelhardt2, Stephan Zahn2, Julian E Fuchs2, Johannes Zuber3,4, Peter Ettmayer2, Mark Pearson2, Mark Petronczki2, Norbert Kraut2, Darryl B McConnell2, Flavio Solca5, Ralph A Neumüller6.
Abstract
Oncogenic alterations in human epidermal growth factor receptor 2 (HER2) occur in approximately 2% of patients with non-small cell lung cancer and predominantly affect the tyrosine kinase domain and cluster in exon 20 of the ERBB2 gene. Most clinical-grade tyrosine kinase inhibitors are limited by either insufficient selectivity against wild-type (WT) epidermal growth factor receptor (EGFR), which is a major cause of dose-limiting toxicity or by potency against HER2 exon 20 mutant variants. Here we report the discovery of covalent tyrosine kinase inhibitors that potently inhibit HER2 exon 20 mutants while sparing WT EGFR, which reduce tumor cell survival and proliferation in vitro and result in regressions in preclinical xenograft models of HER2 exon 20 mutant non-small cell lung cancer, concomitant with inhibition of downstream HER2 signaling. Our results suggest that HER2 exon 20 insertion-driven tumors can be effectively treated by a potent and highly selective HER2 inhibitor while sparing WT EGFR, paving the way for clinical translation.Entities:
Mesh:
Substances:
Year: 2022 PMID: 35883003 DOI: 10.1038/s43018-022-00412-y
Source DB: PubMed Journal: Nat Cancer ISSN: 2662-1347