| Literature DB >> 33863983 |
Takahiro Yoshizawa1,2,3,4, Ken Uchibori1,2, Mitsugu Araki5, Shigeyuki Matsumoto6, Biao Ma7, Ryo Kanada6, Yosuke Seto1, Tomoko Oh-Hara1, Sumie Koike1, Ryo Ariyasu2, Satoru Kitazono2, Hironori Ninomiya8, Kengo Takeuchi8, Noriko Yanagitani2, Satoshi Takagi1, Kazuma Kishi3,4, Naoya Fujita9, Yasushi Okuno5, Makoto Nishio10, Ryohei Katayama11.
Abstract
Approximately 15-30% of patients with lung cancer harbor mutations in the EGFR gene. Major EGFR mutations (>90% of EGFR-mutated lung cancer) are highly sensitive to EGFR tyrosine kinase inhibitors (TKIs). Many uncommon EGFR mutations have been identified, but little is known regarding their characteristics, activation, and sensitivity to various EGFR-TKIs, including allosteric inhibitors. We encountered a case harboring an EGFR-L747P mutation, originally misdiagnosed with EGFR-del19 mutation using a routine diagnostic EGFR mutation test, which was resistant to EGFR-TKI gefitinib. Using this minor mutation and common EGFR-activating mutations, we performed the binding free energy calculations and microsecond-timescale molecular dynamic (MD) simulations, revealing that the L747P mutation considerably stabilizes the active conformation through a salt-bridge formation between K745 and E762. We further revealed why several EGFR inhibitors, including the allosteric inhibitor, were ineffective. Our computational structural analysis strategy would be beneficial for future drug development targeting the EGFR minor mutations.Entities:
Year: 2021 PMID: 33863983 DOI: 10.1038/s41698-021-00170-7
Source DB: PubMed Journal: NPJ Precis Oncol ISSN: 2397-768X