Plasma EGFR T790M ctDNA status is associated with clinical outcome in advanced NSCLC patients with acquired EGFR-TKI resistance

被引:175
作者
Zheng, D. [1 ,4 ]
Ye, X. [2 ]
Zhang, M. Z. [3 ]
Sun, Y. [2 ]
Wang, J. Y. [1 ,4 ]
Ni, J. [1 ,4 ]
Zhang, H. P. [1 ,4 ]
Zhang, L. [1 ,4 ]
Luo, J. [1 ,4 ]
Zhang, J. [1 ,5 ]
Tang, L. [1 ,5 ]
Su, B. [1 ,5 ]
Chen, G. [1 ,6 ]
Zhu, G. [2 ,7 ]
Gu, Y. [2 ]
Xu, J. F. [1 ,4 ]
机构
[1] Tongji Univ, Sch Med, Shanghai Pulm Hosp, Shanghai 200092, Peoples R China
[2] AstraZeneca R&D, Asia & Emerging Markets Innovat Med, Shanghai, Peoples R China
[3] AstraZeneca, Res & Dev Informat, Shanghai, Peoples R China
[4] Shanghai Pulm Hosp, Dept Med Oncol, Xiamen, Peoples R China
[5] Shanghai Pulm Hosp, Cent Lab, Xiamen, Peoples R China
[6] Shanghai Pulm Hosp, Dept Pathol, Xiamen, Peoples R China
[7] Amoy Diagnost, Xiamen, Peoples R China
来源
SCIENTIFIC REPORTS | 2016年 / 6卷
关键词
CELL LUNG-CANCER; GROWTH-FACTOR-RECEPTOR; CIRCULATING TUMOR DNA; INTRATUMOR HETEROGENEITY; NONINVASIVE DETECTION; 1ST-LINE TREATMENT; OPEN-LABEL; MUTATION; GEFITINIB; ERLOTINIB;
D O I
10.1038/srep20913
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
EGFR T790M mutation occurs in half of non-small cell lung cancer (NSCLC) patients with acquired EGFR-TKI (TKI) resistance, based on tumor re-biopsies using an invasive clinical procedure. Here, we dynamically monitored T790M mutation in circulating tumor DNA (ctDNA) using serial plasma samples from NSCLC patients receiving TKI through Droplet Digital PCR (ddPCR) method and the associations between overall survival (OS) starting from initial TKI treatment and the T790M ctDNA status detected in plasma were analyzed. Among 318 patients, 117 who acquired TKI resistance were eligible for the analysis. T790M ctDNA was detected in the plasma of 55/117 (47%) patients. Almost half of the T790M ctDNA positive patients were identified at a median time of 2.2 months prior to clinically progressive disease (PD). Furthermore, within the patients receiving TKI treatment at 2nd line or later, the T790M ctDNA positive group had significantly shorter OS than the negative group (median OS: 26.9 months versus NA, P = 0.0489). Our study demonstrates the feasibility of monitoring EGFR mutation dynamics in serial plasma samples from NSCLC patients receiving TKI therapy. T790M ctDNA can be detected in plasma before and after PD as a poor prognostic factor.
引用
收藏
页数:9
相关论文
共 40 条
  • [1] The Implications of Clonal Genome Evolution for Cancer Medicine
    Aparicio, Samuel
    Caldas, Carlos
    [J]. NEW ENGLAND JOURNAL OF MEDICINE, 2013, 368 (09) : 842 - 851
  • [2] Novel D761Y and common secondary T790M mutations in epidermal growth factor receptor - Mutant lung adenocarcinomas with acquired resistance to kinase inhibitors
    Balak, Marissa N.
    Gong, Yixuan
    Riely, Gregory J.
    Somwar, Romel
    Li, Allan R.
    Zakowski, Maureen F.
    Chiang, Anne
    Yang, Guangli
    Ouerfelli, Ouathek
    Kris, Mark G.
    Ladanyi, Marc
    Miller, Vincent A.
    Pao, William
    [J]. CLINICAL CANCER RESEARCH, 2006, 12 (21) : 6494 - 6501
  • [3] MET amplification occurs with or without T790M mutations in EGFR mutant lung tumors with acquired resistance to gefitinib or erlotinib
    Bean, James
    Brennan, Cameron
    Shih, Jin-Yuan
    Riely, Gregory
    Viale, Agnes
    Wang, Lu
    Chitale, Dhananjay
    Motoi, Noriko
    Szoke, Janos
    Broderick, Stephen
    Balak, Marissa
    Chang, Wen-Cheng
    Yu, Chong-Jen
    Gazdar, Adi
    Pass, Harvey
    Rusch, Valerie
    Gerald, William
    Huang, Shiu-Feng
    Yang, Pan-Chyr
    Miller, Vincent
    Ladany, Marc
    Yang, Chih-Hsin
    Pao, William
    [J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2007, 104 (52) : 20932 - 20937
  • [4] Cancer Genome Scanning in Plasma: Detection of Tumor-Associated Copy Number Aberrations, Single-Nucleotide Variants, and Tumoral Heterogeneity by Massively Parallel Sequencing
    Chan, K. C. Allen
    Jiang, Peiyong
    Zheng, Yama W. L.
    Liao, Gary J. W.
    Sun, Hao
    Wong, John
    Siu, Shing Shun N.
    Chan, Wing C.
    Chan, Stephen L.
    Chan, Anthony T. C.
    Lai, Paul B. S.
    Chiu, Rossa W. K.
    Lo, Y. M. D.
    [J]. CLINICAL CHEMISTRY, 2013, 59 (01) : 211 - 224
  • [5] Clinicopathologic and Molecular Features of Epidermal Growth Factor Receptor T790M Mutation and c-MET Amplification in Tyrosine Kinase Inhibitor-resistant Chinese Non-small Cell Lung Cancer
    Chen, Hua-Jun
    Mok, Tony S.
    Chen, Zhi-Hong
    Guo, Ai-Lin
    Zhang, Xu-Chao
    Su, Jian
    Wu, Yi-Long
    [J]. PATHOLOGY & ONCOLOGY RESEARCH, 2009, 15 (04) : 651 - 658
  • [6] Optimization of Dosing for EGFR-Mutant Non-Small Cell Lung Cancer with Evolutionary Cancer Modeling
    Chmielecki, Juliann
    Foo, Jasmine
    Oxnard, Geoffrey R.
    Hutchinson, Katherine
    Ohashi, Kadoaki
    Somwar, Romel
    Wang, Lu
    Amato, Katherine R.
    Arcila, Maria
    Sos, Martin L.
    Socci, Nicholas D.
    Viale, Agnes
    de Stanchina, Elisa
    Ginsberg, Michelle S.
    Thomas, Roman K.
    Kris, Mark G.
    Inoue, Akira
    Ladanyi, Marc
    Miller, Vincent A.
    Michor, Franziska
    Pao, William
    [J]. SCIENCE TRANSLATIONAL MEDICINE, 2011, 3 (90)
  • [7] Spatial and temporal diversity in genomic instability processes defines lung cancer evolution
    de Bruin, Elza C.
    McGranahan, Nicholas
    Mitter, Richard
    Salm, Max
    Wedge, David C.
    Yates, Lucy
    Jamal-Hanjani, Mariam
    Shafi, Seema
    Murugaesu, Nirupa
    Rowan, Andrew J.
    Groenroos, Eva
    Muhammad, Madiha A.
    Horswell, Stuart
    Gerlinger, Marco
    Varela, Ignacio
    Jones, David
    Marshall, John
    Voet, Thierry
    Van Loo, Peter
    Rassl, Doris M.
    Rintoul, Robert C.
    Janes, Sam M.
    Lee, Siow-Ming
    Forster, Martin
    Ahmad, Tanya
    Lawrence, David
    Falzon, Mary
    Capitanio, Arrigo
    Harkins, Timothy T.
    Lee, Clarence C.
    Tom, Warren
    Teefe, Enock
    Chen, Shann-Ching
    Begum, Sharmin
    Rabinowitz, Adam
    Phillimore, Benjamin
    Spencer-Dene, Bradley
    Stamp, Gordon
    Szallasi, Zoltan
    Matthews, Nik
    Stewart, Aengus
    Campbell, Peter
    Swanton, Charles
    [J]. SCIENCE, 2014, 346 (6206) : 251 - 256
  • [8] MET amplification leads to gefitinib resistance in lung cancer by activating ERBB3 signaling
    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.
    [J]. SCIENCE, 2007, 316 (5827) : 1039 - 1043
  • [9] Intratumor Heterogeneity and Branched Evolution Revealed by Multiregion Sequencing
    Gerlinger, Marco
    Rowan, Andrew J.
    Horswell, Stuart
    Larkin, James
    Endesfelder, David
    Gronroos, Eva
    Martinez, Pierre
    Matthews, Nicholas
    Stewart, Aengus
    Tarpey, Patrick
    Varela, Ignacio
    Phillimore, Benjamin
    Begum, Sharmin
    McDonald, Neil Q.
    Butler, Adam
    Jones, David
    Raine, Keiran
    Latimer, Calli
    Santos, Claudio R.
    Nohadani, Mahrokh
    Eklund, Aron C.
    Spencer-Dene, Bradley
    Clark, Graham
    Pickering, Lisa
    Stamp, Gordon
    Gore, Martin
    Szallasi, Zoltan
    Downward, Julian
    Futreal, P. Andrew
    Swanton, Charles
    [J]. NEW ENGLAND JOURNAL OF MEDICINE, 2012, 366 (10) : 883 - 892
  • [10] EGFR-Driven Behavior and Intrapatient T790M Mutation Heterogeneity of Non-Small-Cell Carcinoma With Squamous Histology
    Graziano, Paolo
    de Marinis, Filippo
    Gori, Bruno
    Gasbarra, Rita
    Migliorino, Rita
    De Santis, Stefano
    Pelosi, Giuseppe
    Leone, Alvaro
    [J]. JOURNAL OF CLINICAL ONCOLOGY, 2015, 33 (31) : E115 - E118
1234