Landscape of EGFR-Dependent and -Independent Resistance Mechanisms to Osimertinib and Continuation Therapy Beyond Progression in -Mutant NSCLC

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2018 Sep 20

PMID 30228210

Citations 203

Authors

Xiuning Le

Sonam Puri

Marcelo V Negrao

Monique B Nilsson

Jacqulyne Robichaux

Theresa Boyle

J Kevin Hicks

Katherine L Lovinger

Emily Roarty

Waree Rinsurongkawong

Ming Tang

Huiying Sun

Yasir Elamin

Lara C Lacerda

Jeff Lewis

Jack A Roth

Stephen G Swisher

J Jack Lee

William N William Jr

Bonnie S Glisson

Jianjun Zhang

Vassiliki A Papadimitrakopoulou

Jhanelle E Gray

John V Heymach

Affiliations

Soon will be listed here.

Abstract

Purpose: Osimertinib was initially approved for T790M-positive non-small cell lung cancer (NSCLC) and, more recently, for first-line treatment of -mutant NSCLC. However, resistance mechanisms to osimertinib have been incompletely described.

Experimental Design: Using cohorts from The University of Texas MD Anderson Lung Cancer Moonshot GEMINI and Moffitt Cancer Center lung cancer databases, we collected clinical data for patients treated with osimertinib. Molecular profiling analysis was performed at the time of progression in a subset of the patients.

Results: In the 118 patients treated with osimertinib, 42 had molecular profiling at progression. T790M was preserved in 21 (50%) patients and lost in 21 (50%). EGFR C797 and L792 (26%) mutations were the most common resistance mechanism and were observed exclusively in T790M-preserved cases. MET amplification was the second most common alteration (14%). Recurrent alterations were observed in 22 genes/pathways, including PIK3CA, FGFR, and RET. Preclinical studies confirmed MET, PIK3CA, and epithelial-to-mesenchymal transition as potential resistance drivers. Alterations of cell-cycle genes were associated with shorter median progression-free survival (PFS, 4.4 vs. 8.8 months, = 0.01). In 76 patients with progression, osimertinib was continued in 47 cases with a median second PFS (PFS2) of 12.6 months; 21 patients received local consolidation radiation with a median PFS of 15.5 months. Continuation of osimertinib beyond progression was associated with a longer overall survival compared with discontinuation (11.2 vs. 6.1 months, = 0.02).

Conclusions: Osimertinib resistance is associated with diverse, predominantly EGFR-independent genomic alterations. Continuation of osimertinib after progression, alone or in conjunction with radiotherapy, may provide prolonged clinical benefit in selected patients..

Citing Articles

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