Crizotinib treatment for patients with EGFR mutation positive NSCLC that acquire cMET amplification after EGFR TKI therapy results in short-lived and heterogeneous responses

被引:16
作者
van Veggel, Bianca [1 ]
de Langen, Adrianus J. [1 ]
Hashemi, Sayed [2 ]
Monkhorst, Kim [3 ]
Rosenberg, Efraim H. [3 ]
Heideman, Danielle A. M. [4 ]
Radonic, Teodora [4 ]
Smit, Egbert F. [1 ,2 ]
机构
[1] Antoni van Leeuwenhoek Hosp, Dept Thorac Oncol, Netherlands Canc Inst, Plesmanlaan 121, NL-1066 CX Amsterdam, Netherlands
[2] Vrije Univ Amsterdam Med Ctr, Dept Pulm Dis, Boelelaan 1117, NL-1081 HV Amsterdam, Netherlands
[3] Antoni van Leeuwenhoek Hosp, Netherlands Canc Inst, Dept Pathol, Plesmanlaan 121, NL-1066 CX Amsterdam, Netherlands
[4] Vrije Univ Amsterdam Med Ctr, Canc Ctr Amsterdam, Dept Pathol, Boelelaan 1117, NL-1081 HV Amsterdam, Netherlands
来源
LUNG CANCER | 2018年 / 124卷
关键词
EGFR mutation; cMET amplification; Resistance; Crizotinib; CELL LUNG-CANCER; MET AMPLIFICATION; RESISTANCE MECHANISMS; OSIMERTINIB; PROGRESSION; INHIBITORS;
D O I
10.1016/j.lungcan.2018.07.030
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Purpose: Next to secondary epidermal growth factor receptor (EGFR) mutations, cMET amplification plays an important role in mediating acquired resistance to EGFR tyrosine kinase inhibitors (TKI) treatment. Crizotinib, a dual ALK and cMET inhibitor, can induce responses in patients with EGFR mutation positive non-small cell lung cancer (NSCLC) that acquire cMET amplification after EGFR TM treatment. However, little is known about the duration of response and post-progression resistance mechanisms. Here, we report on the clinical outcome of a series of patients with cMET-driven resistance to EGFR TKIs, treated with crizotinib. Materials and methods: Eight patients with EGFR mutation positive NSCLC that acquired cMET amplification after EGFR TKI treatment were treated with crizotinib 250 mg twice daily, as monotherapy (n = 2) or in combination with an EGFR TKI (n = 6). Results: Four out of eight patients (50%) showed a partial response (PR) according to RECIST 1.1. Median progression-free survival (PFS) was 1.4 (95% CI 1.2-5.0) months. Responses were short-lasting with a median PFS of 3.5 (95% CI 1.4-5.2) months in patients with a PR. Median overall survival was 5.9 (95% CI 1.3-6.0) months and not statistically different between responders and non-responders (p = 0.37). All but one patient tolerated crizotinib treatment well. Heterogeneous responses were seen in patients with progressive disease as best response with a marked size decrease of the biopsied (cMET amplification positive) lesion and progression of other lesions. cMET amplification was not always mutually exclusive with other EGFR TKI resistance mechanisms. Post-progression biopsies were negative for cMET amplification. Conclusion: Crizotinib treatment for patients with EGFR mutation positive NSCLC that acquire cMET amplification after EGFR TKI treatment results in short-lived and often heterogeneous responses, possibly due to subclonality of cMET-driven resistance and co-occurrence of other EGFR TKI resistance mechanisms.
引用
收藏
页码:130 / 134
页数:5
相关论文
共 17 条
[1]   Outcome of EGFR-mutated NSCLC patients with MET-driven resistance to EGFR tyrosine kinase inhibitors [J].
Baldacci, Simon ;
Mazieres, Julien ;
Tomasini, Pascale ;
Girard, Nicolas ;
Guisier, Florian ;
Audigier-Valette, Clarisse ;
Monnet, Isabelle ;
Wislez, Marie ;
Perol, Maurice ;
Do, Pascal ;
Dansin, Eric ;
Leduc, Charlotte ;
Leprieur, Etienne Giroux ;
Moro-Sibilot, Denis ;
Tulasne, David ;
Kherrouche, Zoulika ;
Labreuche, Julien ;
Cortot, Alexis B. .
ONCOTARGET, 2017, 8 (62) :105103-105114
[2]   Prevalence and clinical association of MET gene overexpression and amplification in patients with NSCLC: Results from the European Thoracic Oncology Platform (ETOP) Lungscape project [J].
Bubendorf, Lukas ;
Dafni, Urania ;
Schobel, Martin ;
Finn, Stephen P. ;
Tischler, Verena ;
Sejda, Aleksandra ;
Marchetti, Antonio ;
Thunnissen, Erik ;
Verbeken, Eric K. ;
Warth, Arne ;
Sansano, Irene ;
Cheney, Richard ;
Speel, Ernst Jan M. ;
Nonaka, Daisuke ;
Monkhorst, Kim ;
Hager, Henrik ;
Martorell, Miguel ;
Savic, Spasenija ;
Kerr, Keith M. ;
Tan, Qiang ;
Tsourti, Zoi ;
Geiger, Thomas R. ;
Kammler, Roswitha ;
Schulze, Katja ;
Das-Gupta, Ashis ;
Shames, David ;
Peters, Solange ;
Stahel, Rolf A. .
LUNG CANCER, 2017, 111 :143-149
[3]   Circulating tumour DNA profiling reveals heterogeneity of EGFR inhibitor resistance mechanisms in lung cancer patients [J].
Chabon, Jacob J. ;
Simmons, Andrew D. ;
Lovejoy, Alexander F. ;
Esfahani, Mohammad S. ;
Newman, Aaron M. ;
Haringsma, Henry J. ;
Kurtz, David M. ;
Stehr, Henning ;
Scherer, Florian ;
Karlovich, Chris A. ;
Harding, Thomas C. ;
Durkin, Kathleen A. ;
Otterson, Gregory A. ;
Purcell, W. Thomas ;
Camidge, D. Ross ;
Goldman, Jonathan W. ;
Sequist, Lecia V. ;
Piotrowska, Zofia ;
Wakelee, Heather A. ;
Neal, Joel W. ;
Alizadeh, Ash A. ;
Diehn, Maximilian .
NATURE COMMUNICATIONS, 2016, 7
[4]   MET amplification leads to gefitinib resistance in lung cancer by activating ERBB3 signaling [J].
Engelman, Jeffrey A. ;
Zejnullahu, Kreshnik ;
Mitsudomi, Tetsuya ;
Song, Youngchul ;
Hyland, Courtney ;
Park, Joon Oh ;
Lindeman, Neal ;
Gale, Christopher-Michael ;
Zhao, Xiaojun ;
Christensen, James ;
Kosaka, Takayuki ;
Holmes, Alison J. ;
Rogers, Andrew M. ;
Cappuzzo, Federico ;
Mok, Tony ;
Lee, Charles ;
Johnson, Bruce E. ;
Cantley, Lewis C. ;
Janne, Pasi A. .
SCIENCE, 2007, 316 (5827) :1039-1043
[5]   Simultaneous Detection of Clinically Relevant Mutations and Amplifications for Routine Cancer Pathology [J].
Hoogstraat, Marlous ;
Hinrichs, John W. J. ;
Besselink, Nicolle J. M. ;
Radersma-van Loon, Joyce H. ;
de Voijs, Carmen M. A. ;
Peeters, Ton ;
Nijman, Isaac J. ;
de Weger, Roel A. ;
Voest, Emile E. ;
Willems, Stefan M. ;
Cuppen, Edwin ;
Koudijs, Marco J. .
JOURNAL OF MOLECULAR DIAGNOSTICS, 2015, 17 (01) :10-18
[6]   Impact of EGFR Inhibitor in Non-Small Cell Lung Cancer on Progression-Free and Overall Survival: A Meta-Analysis [J].
Lee, Chee Khoon ;
Brown, Chris ;
Gralla, Richard J. ;
Hirsh, Vera ;
Thongprasert, Sumitra ;
Tsai, Chun-Ming ;
Tan, Eng Huat ;
Ho, James Chung-Man ;
Chu, Da Tong ;
Zaatar, Adel ;
Osorio Sanchez, Jemela Anne ;
Vu Van Vu ;
Au, Joseph Siu Kie ;
Inoue, Akira ;
Lee, Siow Ming ;
Gebski, Val ;
Yang, James Chih-Hsin .
JNCI-JOURNAL OF THE NATIONAL CANCER INSTITUTE, 2013, 105 (09) :595-605
[7]   Acquired MET Y1248H and D1246N Mutations Mediate Resistance to MET Inhibitors in Non-Small Cell Lung Cancer [J].
Li, Anna ;
Yang, Jin-ji ;
Zhang, Xu-chao ;
Zhang, Zhou ;
Su, Jian ;
Gou, Lan-ying ;
Bai, Yu ;
Zhou, Qing ;
Yang, Zhenfan ;
Han Han-Zhang ;
Zhong, Wen-Zhao ;
Chuai, Shannon ;
Zhang, Qi ;
Xie, Zhi ;
Gao, Hongfei ;
Chen, Huajun ;
Wang, Zhen ;
Wang, Zheng ;
Yang, Xue-ning ;
Wang, Bin-chao ;
Gan, Bin ;
Chen, Zhi-hong ;
Jiang, Ben-yuan ;
Wu, Si-pei ;
Liu, Si-yang ;
Xu, Chong-rui ;
Wu, Yi-long .
CLINICAL CANCER RESEARCH, 2017, 23 (16) :4929-4937
[8]  
Minari R., 2018, J THORAC ONCOL OFF P
[9]   High MET amplification level as a resistance mechanism to osimertinib (AZD9291) in a patient that symptomatically responded to crizotinib treatment post-osimertinib progression [J].
Ou, Sai-Hong Ignatius ;
Agarwal, Nikita ;
Ali, Siraj M. .
LUNG CANCER, 2016, 98 :59-61
[10]   MET amplification (amp) as a resistance mechanism to osimertinib. [J].
Piotrowska, Zofia ;
Thress, Kenneth Stephen ;
Mooradian, Meghan ;
Heist, Rebecca Suk ;
Azzoli, Christopher G. ;
Temel, Jennifer S. ;
Rizzo, Coleen ;
Nagy, Rebecca J. ;
Lanman, Richard B. ;
Gettinger, Scott N. ;
Evans, Tracey L. ;
Hata, Aaron N. ;
Shaw, Alice Tsang ;
Sequist, Lecia V. .
JOURNAL OF CLINICAL ONCOLOGY, 2017, 35
12