Real-World Data on Combined EGFR-TKI and Crizotinib Treatment for Acquired and De Novo MET Amplification in Patients with Metastatic EGFR-Mutated NSCLC

Edyta M Urbanska; Morten Grauslund; Peter R Koffeldt; Sarah L B Truelsen; Johan O Löfgren; Junia C Costa; Linea C Melchior; Jens B Sørensen; Eric Santoni-Rugiu

doi:10.3390/ijms241713077

Real-World Data on Combined EGFR-TKI and Crizotinib Treatment for Acquired and De Novo MET Amplification in Patients with Metastatic EGFR-Mutated NSCLC

Int J Mol Sci. 2023 Aug 23;24(17):13077. doi: 10.3390/ijms241713077.

Authors

Affiliations

¹ Department of Oncology, Rigshospitalet, Copenhagen University Hospital, DK-2100 Copenhagen, Denmark.
² Department of Pathology, Rigshospitalet, Copenhagen University Hospital, DK-2100 Copenhagen, Denmark.
³ Department of Clinical Physiology and Nuclear Medicine, Rigshospitalet, Copenhagen University Hospital, DK-2100 Copenhagen, Denmark.
⁴ Department of Radiology, Rigshospitalet, Copenhagen University Hospital, DK-2100 Copenhagen, Denmark.
⁵ Department of Clinical Medicine, University of Copenhagen, DK-2200 Copenhagen, Denmark.

Abstract

Amplification of the mesenchymal epithelial transition (MET) gene is a mechanism of acquired resistance to epidermal growth factor receptor (EGFR)-tyrosine-kinase-inhibitors (TKIs) in over 20% of patients with advanced EGFR-mutated (EGFRm+) non-small lung cancer (NSCLC). However, it may also occur de novo in 2-8% of EGFRm+ NSCLC cases as a potential mechanism of intrinsic resistance. These patients represent a group with unmet needs, since there is no standard therapy currently approved. Several new MET inhibitors are being investigated in clinical trials, but the results are awaited. Meanwhile, as an alternative strategy, combinations of EGFR-TKIs with the MET/ALK/ROS1-TKI Crizotinib may be used in this setting, despite this use is principally off-label. Thus, we studied five of these MET amplified cases receiving EGFR-TKI and Crizotinib doublet after progression on EGFR-TKI treatment to assess the benefits and challenges related to this combination and the possible occurrence of genomic and phenotypic co-alterations. Furthermore, we compared our cases with other real-world reports on Crizotinib/EGFR-TKI combinations, which appeared effective, especially in patients with high-level MET amplification. Yet, we observed that the co-occurrence of other genomic and phenotypical alterations may affect the response to combined EGFR-TKI and Crizotinib. Finally, given the heterogeneity of MET amplification, the diagnostic methods for assessing it may be discrepant. In this respect, we observed that for optimal detection, immunohistochemistry, fluorescence in situ hybridization, and next-generation sequencing should be used together, as these methods possess different sensitivities and complement each other in characterizing MET amplification. Additionally, we addressed the issue of managing EGFR-mutated NSCLC patients with de novo MET amplification causing primary EGFR-TKI resistance. We conclude that, while data from clinical trials with new MET inhibitors are still pending, adding Crizotinib to EGFR-TKI in NSCLC patients acquiring MET amplification at progression on EGFR-TKI monotherapy is a reasonable approach, with a progression-free survival of 3-19 months.

Keywords: Crizotinib; EGFR-TKI; EGFR-mutated NSCLC; acquired MET amplification; combined targeted therapy; de novo MET amplification.

MeSH terms

Crizotinib / therapeutic use
ErbB Receptors / genetics
Humans
In Situ Hybridization, Fluorescence
Lung Neoplasms* / drug therapy
Lung Neoplasms* / genetics
Proto-Oncogene Proteins c-met / genetics
Tyrosine Kinase Inhibitors* / pharmacology

Substances

Crizotinib
EGFR protein, human
ErbB Receptors
Proto-Oncogene Proteins c-met
Tyrosine Kinase Inhibitors

Grants and funding

This research received no external funding.