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Data from Drug Sensitivity and Allele Specificity of First-Line Osimertinib Resistance EGFR Mutations

Posted on 2023-03-31 - 03:06
Abstract

Osimertinib, a mutant-specific third-generation EGFR tyrosine kinase inhibitor, is emerging as the preferred first-line therapy for EGFR-mutant lung cancer, yet resistance inevitably develops in patients. We modeled acquired resistance to osimertinib in transgenic mouse models of EGFRL858R-induced lung adenocarcinoma and found that it is mediated largely through secondary mutations in EGFR—either C797S or L718V/Q. Analysis of circulating free DNA data from patients revealed that L718Q/V mutations almost always occur in the context of an L858R driver mutation. Therapeutic testing in mice revealed that both erlotinib and afatinib caused regression of osimertinib-resistant C797S-containing tumors, whereas only afatinib was effective on L718Q mutant tumors. Combination first-line osimertinib plus erlotinib treatment prevented the emergence of secondary mutations in EGFR. These findings highlight how knowledge of the specific characteristics of resistance mutations is important for determining potential subsequent treatment approaches and suggest strategies to overcome or prevent osimertinib resistance in vivo.

Significance:

This study provides insight into the biological and molecular properties of osimertinib resistance EGFR mutations and evaluates therapeutic strategies to overcome resistance.

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FUNDING

Yale's Specialized Program of Research Excellence in Lung Cancer

AstraZeneca

NIH

NCI

Lung Cancer Research

Canadian Institutes of Health Research

Michael Smith Foundation

NIHR New Investigator Awards

the IMED AstraZeneca postdoc program

CIHR

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Cancer Research

AUTHORS (24)

  • Jacqueline H. Starrett
    Alexis A. Guernet
    Maria Emanuela Cuomo
    Kamrine E. Poels
    Iris K. van Alderwerelt van Rosenburgh
    Amy Nagelberg
    Dylan Farnsworth
    Kristin S. Price
    Hina Khan
    Kumar Dilip Ashtekar
    Mmaserame Gaefele
    Deborah Ayeni
    Tyler F. Stewart
    Alexandra Kuhlmann
    Susan M. Kaech
    Arun M. Unni
    Robert Homer
    William W. Lockwood
    Franziska Michor
    Sarah B. Goldberg
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