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Dynamics of multiple resistance mechanisms in plasma DNA during EGFR‐targeted therapies in non‐small cell lung cancer

Authors :
Dana Wai Yi Tsui
Muhammed Murtaza
Alvin Seng Cheong Wong
Oscar M Rueda
Christopher G Smith
Dineika Chandrananda
Ross A Soo
Hong Liang Lim
Boon Cher Goh
Carlos Caldas
Tim Forshew
Davina Gale
Wei Liu
James Morris
Francesco Marass
Tim Eisen
Tan Min Chin
Nitzan Rosenfeld
Source :
EMBO Molecular Medicine, Vol 10, Iss 6, Pp 1-14 (2018)
Publication Year :
2018
Publisher :
Springer Nature, 2018.

Abstract

Abstract Tumour heterogeneity leads to the development of multiple resistance mechanisms during targeted therapies. Identifying the dominant driver(s) is critical for treatment decision. We studied the relative dynamics of multiple oncogenic drivers in longitudinal plasma of 50 EGFR‐mutant non‐small‐cell lung cancer patients receiving gefitinib and hydroxychloroquine. We performed digital PCR and targeted sequencing on samples from all patients and shallow whole‐genome sequencing on samples from three patients who underwent histological transformation to small‐cell lung cancer. In 43 patients with known EGFR mutations from tumour, we identified them accurately in plasma of 41 patients (95%, 41/43). We also found additional mutations, including EGFR T790M (31/50, 62%), TP53 (23/50, 46%), PIK3CA (7/50, 14%) and PTEN (4/50, 8%). Patients with both TP53 and EGFR mutations before treatment had worse overall survival than those with only EGFR. Patients who progressed without T790M had worse PFS during TKI continuation and developed alternative alterations, including small‐cell lung cancer‐associated copy number changes and TP53 mutations, that tracked subsequent treatment responses. Longitudinal plasma analysis can help identify dominant resistance mechanisms, including non‐druggable genetic information that may guide clinical management.

Details

Language :
English
ISSN :
17574676 and 17574684
Volume :
10
Issue :
6
Database :
Directory of Open Access Journals
Journal :
EMBO Molecular Medicine
Publication Type :
Academic Journal
Accession number :
edsdoj.359abd7345a3480bbf157d3f3b813302
Document Type :
article
Full Text :
https://doi.org/10.15252/emmm.201707945