MET Exon 14 Mutations in Non-Small-Cell Lung Cancer Are Associated With Advanced Age and Stage-Dependent MET Genomic Amplification and c-Met Overexpression

被引:564
作者
Awad, Mark M. [1 ,2 ,3 ]
Oxnard, Geoffrey R. [1 ,2 ,3 ]
Jackman, David M. [1 ,2 ,3 ]
Savukoski, Daniel O. [2 ,3 ]
Hall, Dimity [2 ,3 ]
Shivdasani, Priyanka [2 ,3 ]
Heng, Jennifer C. [1 ]
Dahlberg, Suzanne E. [1 ]
Anne, Pasi A. J. [1 ,2 ,3 ]
Verma, Suman [4 ]
Christensen, James [5 ]
Hammerman, Peter S. [1 ,2 ,3 ]
Sholl, Lynette M. [2 ,3 ]
机构
[1] Dana Farber Canc Inst, 450 Brookline Ave,D1240G, Boston, MA 02215 USA
[2] Brigham & Womens Hosp, 75 Francis St, Boston, MA 02115 USA
[3] Harvard Univ, Sch Med, Boston, MA USA
[4] ResearchDX, Irvine, CA USA
[5] Mirati Therapeut, San Diego, CA USA
来源
JOURNAL OF CLINICAL ONCOLOGY | 2016年 / 34卷 / 07期
关键词
ANAPLASTIC LYMPHOMA KINASE; HEPATOCYTE GROWTH-FACTOR; MISSENSE MUTATION; LAST NUCLEOTIDE; GENE FUSIONS; ALK; ROS1; FEATURES; SPLICE; DOMAIN;
D O I
10.1200/JCO.2015.63.4600
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Purpose Non-small-cell lung cancers (NSCLCs) harboring mutations in MET exon 14 and its flanking introns may respond to c-Met inhibitors. We sought to describe the clinical, pathologic, and genomic characteristics of patients with cancer with MET exon 14 mutations. Patients and Methods We interrogated next-generation sequencing results from 6,376 cancers to identify those harboring MET exon 14 mutations. Clinical characteristics of MET exon 14 mutated NSCLCs were compared with those of NSCLCs with activating mutations in KRAS and EGFR. Co-occurring genomic mutations and copy number alterations were identified. c-Met immunohistochemistry and real-time polymerase chain reaction to detect exon 14 skipping were performed where sufficient tissue was available. Results MET exon 14 mutations were identified in 28 of 933 nonsquamous NSCLCs (3.0%) and were not seen in other cancer types in this study. Patients with MET exon 14-mutated NSCLC were significantly older (median age, 72.5 years) than patients with EGFR-mutant (median age, 61 years; P < .001) or KRAS-mutant NSCLC (median age, 65 years; P,.001). Among patients with MET exon 14 mutations, 68% were women, and 36% were never-smokers. Stage IV MET exon 14-mutated NSCLCs were significantly more likely to have concurrent MET genomic amplification (mean ratio of MET to chromosome 7, 4.3) and strong c-Met immunohistochemical expression (mean H score, 253) than stage IA to IIIB MET exon 14-mutated NSCLCs (mean ratio of MET to chromosome 7, 1.4; P = .007; mean H score, 155; P = .002) and stage IV MET exon 14-wild-type NSCLCs (mean ratio of MET to chromosome 7, 1.2; P < .001; mean H score, 142; P < .001). A patient whose lung cancer harbored a MET exon 14 mutation with concurre nt genomic amplification of the mutated MET allele experienced a major partial response to the c-Met inhibitor crizotinib. Conclusion MET exon 14 mutations represent a clinically unique molecular subtype of NSCLC. Prospective clinical trials with c-Met inhibitors will be necessary to validate MET exon 14 mutations as an important therapeutic target in NSCLC. (C) 2016 by American Society of Clinical Oncology
引用
收藏
页码:721 / +
页数:13
相关论文
共 47 条
[11]   Response to Crizotinib in a Patient With Lung Adenocarcinoma Harboring a MET Splice Site Mutation [J].
Jenkins, Russell W. ;
Oxnard, Geoffrey R. ;
Elkin, Sheryl ;
Sullivan, E. Kelly ;
Carter, Jennifer L. ;
Barbie, David A. .
CLINICAL LUNG CANCER, 2015, 16 (05) :E101-E104
[12]   A G to A transition at the last nucleotide of exon 6 of the γc gene (868G→A) may result in either a splice or missense mutation in patients with X-linked severe combined immunodeficiency [J].
Kanai, N ;
Yanai, F ;
Hirose, S ;
Nibu, K ;
Izuhara, K ;
Tani, T ;
Kubota, T ;
Mitsudome, A .
HUMAN GENETICS, 1999, 104 (01) :36-42
[13]   KIF5B-RET fusions in lung adenocarcinoma [J].
Kohno, Takashi ;
Ichikawa, Hitoshi ;
Totoki, Yasushi ;
Yasuda, Kazuki ;
Hiramoto, Masaki ;
Nammo, Takao ;
Sakamoto, Hiromi ;
Tsuta, Koji ;
Furuta, Koh ;
Shimada, Yoko ;
Iwakawa, Reika ;
Ogiwara, Hideaki ;
Oike, Takahiro ;
Enari, Masato ;
Schetter, Aaron J. ;
Okayama, Hirokazu ;
Haugen, Aage ;
Skaug, Vidar ;
Chiku, Suenori ;
Yamanaka, Itaru ;
Arai, Yasuhito ;
Watanabe, Shun-ichi ;
Sekine, Ikuo ;
Ogawa, Seishi ;
Harris, Curtis C. ;
Tsuda, Hitoshi ;
Yoshida, Teruhiko ;
Yokota, Jun ;
Shibata, Tatsuhiro .
NATURE MEDICINE, 2012, 18 (03) :375-377
[14]   Somatic mutations lead to an oncogenic deletion of Met in lung cancer [J].
Kong-Beltran, M ;
Seshagiri, S ;
Zha, JP ;
Zhu, WJ ;
Bhawe, K ;
Mendoza, N ;
Holcomb, T ;
Pujara, K ;
Stinson, J ;
Fu, L ;
Severin, C ;
Rangell, L ;
Schwall, R ;
Amler, L ;
Wickramasinghe, D ;
Yauch, R .
CANCER RESEARCH, 2006, 66 (01) :283-289
[15]   Anaplastic Lymphoma Kinase Inhibition in Non-Small-Cell Lung Cancer [J].
Kwak, Eunice L. ;
Bang, Yung-Jue ;
Camidge, D. Ross ;
Shaw, Alice T. ;
Solomon, Benjamin ;
Maki, Robert G. ;
Ou, Sai-Hong I. ;
Dezube, Bruce J. ;
Jaenne, Pasi A. ;
Costa, Daniel B. ;
Varella-Garcia, Marileila ;
Kim, Woo-Ho ;
Lynch, Thomas J. ;
Fidias, Panos ;
Stubbs, Hannah ;
Engelman, Jeffrey A. ;
Sequist, Lecia V. ;
Tan, WeiWei ;
Gandhi, Leena ;
Mino-Kenudson, Mari ;
Wei, Greg C. ;
Shreeve, S. Martin ;
Ratain, Mark J. ;
Settleman, Jeffrey ;
Christensen, James G. ;
Haber, Daniel A. ;
Wilner, Keith ;
Salgia, Ravi ;
Shapiro, Geoffrey I. ;
Clark, Jeffrey W. ;
Iafrate, A. John .
NEW ENGLAND JOURNAL OF MEDICINE, 2010, 363 (18) :1693-1703
[16]  
Laurance WF, 2014, NATURE, V514, P262, DOI 10.1038/nature13876
[17]   Identification of new ALK and RET gene fusions from colorectal and lung cancer biopsies [J].
Lipson, Doron ;
Capelletti, Marzia ;
Yelensky, Roman ;
Otto, Geoff ;
Parker, Alex ;
Jarosz, Mirna ;
Curran, John A. ;
Balasubramanian, Sohail ;
Bloom, Troy ;
Brennan, Kristina W. ;
Donahue, Amy ;
Downing, Sean R. ;
Frampton, Garrett M. ;
Garcia, Lazaro ;
Juhn, Frank ;
Mitchell, Kathy C. ;
White, Emily ;
White, Jared ;
Zwirko, Zac ;
Peretz, Tamar ;
Nechushtan, Hovav ;
Soussan-Gutman, Lior ;
Kim, Jhingook ;
Sasaki, Hidefumi ;
Kim, Hyeong Ryul ;
Park, Seung-il ;
Ercan, Dalia ;
Sheehan, Christine E. ;
Ross, Jeffrey S. ;
Cronin, Maureen T. ;
Jaenne, Pasi A. ;
Stephens, Philip J. .
NATURE MEDICINE, 2012, 18 (03) :382-384
[18]   Molecular Pathways: Resistance to Kinase Inhibitors and Implications for Therapeutic Strategies [J].
Lovly, Christine M. ;
Shaw, Alice T. .
CLINICAL CANCER RESEARCH, 2014, 20 (09) :2249-2256
[19]   Activating mutations in the epidermal growth factor receptor underlying responsiveness of non-small-cell lung cancer to gefitinib [J].
Lynch, TJ ;
Bell, DW ;
Sordella, R ;
Gurubhagavatula, S ;
Okimoto, RA ;
Brannigan, BW ;
Harris, PL ;
Haserlat, SM ;
Supko, JG ;
Haluska, FG ;
Louis, DN ;
Christiani, DC ;
Settleman, J ;
Haber, DA .
NEW ENGLAND JOURNAL OF MEDICINE, 2004, 350 (21) :2129-2139
[20]   Functional expression and mutations of c-met and its therapeutic inhibition with SU11274 and small interfering RNA in non-small cell lung cancer [J].
Ma, PC ;
Jagadeeswaran, R ;
Jagadeesh, S ;
Tretiakova, MS ;
Nallasura, V ;
Fox, EA ;
Hansen, M ;
Schaefer, E ;
Naoki, K ;
Lader, A ;
Richards, W ;
Sugarbaker, D ;
Husain, AN ;
Christensen, JG ;
Salgia, R .
CANCER RESEARCH, 2005, 65 (04) :1479-1488
12345