| Literature DB >> 33654076 |
Zhenfang Du1, Benjamin P Brown2,3,4, Soyeon Kim5, Donna Ferguson6, Dean C Pavlick7, Gowtham Jayakumaran6, Ryma Benayed6, Jean-Nicolas Gallant1, Yun-Kai Zhang1, Yingjun Yan1, Monica Red-Brewer1, Siraj M Ali7, Alexa B Schrock7, Ahmet Zehir6, Marc Ladanyi6, Adam W Smith5, Jens Meiler8,9,10, Christine M Lovly11,12.
Abstract
Mechanistic understanding of oncogenic variants facilitates the development and optimization of treatment strategies. We recently identified in-frame, tandem duplication of EGFR exons 18 - 25, which causes EGFR Kinase Domain Duplication (EGFR-KDD). Here, we characterize the prevalence of ERBB family KDDs across multiple human cancers and evaluate the functional biochemistry of EGFR-KDD as it relates to pathogenesis and potential therapeutic intervention. We provide computational and experimental evidence that EGFR-KDD functions by forming asymmetric EGF-independent intra-molecular and EGF-dependent inter-molecular dimers. Time-resolved fluorescence microscopy and co-immunoprecipitation reveals EGFR-KDD can form ligand-dependent inter-molecular homo- and hetero-dimers/multimers. Furthermore, we show that inhibition of EGFR-KDD activity is maximally achieved by blocking both intra- and inter-molecular dimerization. Collectively, our findings define a previously unrecognized model of EGFR dimerization, providing important insights for the understanding of EGFR activation mechanisms and informing personalized treatment of patients with tumors harboring EGFR-KDD. Finally, we establish ERBB KDDs as recurrent oncogenic events in multiple cancers.Entities:
Year: 2021 PMID: 33654076 DOI: 10.1038/s41467-021-21613-6
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919