Mutations in the DDR2 Kinase Gene identify a Novel therapeutic target in squamous cell lung cancer

被引:375
作者
Hammerman, Peter S. [1 ]
Sos, Martin L. [6 ,7 ,8 ,9 ]
Ramos, Alex H. [5 ]
Xu, Chunxiao [1 ]
Dutt, Amit [5 ]
Zhou, Wenjun [2 ]
Brace, Lear E. [1 ]
Woods, Brittany A. [1 ]
Lin, Wenchu [1 ]
Zhang, Jianming [2 ]
Deng, Xianming [2 ]
Lim, Sang Min [2 ]
Heynck, Stefanie [6 ,7 ]
Peifer, Martin [6 ,7 ]
Simard, Jeffrey R. [12 ]
Lawrence, Michael S. [5 ]
Onofrio, Robert C. [5 ]
Salvesen, Helga B. [15 ,16 ]
Seidel, Danila [6 ,7 ]
Zander, Thomas [8 ,9 ,10 ]
Heuckmann, Johannes M. [6 ,7 ]
Soltermann, Alex [18 ]
Moch, Holger [18 ]
Koker, Mirjam [6 ,7 ]
Leenders, Frauke [6 ,7 ]
Gabler, Franziska [6 ,7 ]
Querings, Silvia [6 ,7 ]
Ansen, Sascha [10 ]
Brambilla, Elisabeth [19 ]
Brambilla, Christian [19 ]
Lorimier, Philippe [19 ]
Brustugun, Odd Terje [17 ]
Helland, Aslaug [17 ]
Petersen, Iver [14 ]
Clement, Joachim H. [14 ]
Groen, Harry [20 ,21 ,22 ]
Timens, Wim [20 ,21 ,22 ]
Sietsma, Hannie [20 ,21 ,22 ]
Stoelben, Erich [11 ]
Wolf, Juergen [8 ,9 ,10 ]
Beer, David G. [23 ]
Tsao, Ming Sound [24 ,25 ]
Hanna, Megan [1 ,3 ,5 ]
Hatton, Charles [1 ,3 ,5 ]
Eck, Michael J. [1 ]
Janne, Pasi A. [1 ]
Johnson, Bruce E. [1 ]
Winckler, Wendy [5 ]
Greulich, Heidi [1 ,5 ]
Bass, Adam J. [1 ]
机构
[1] Dana Farber Canc Inst, Dept Med Oncol, Boston, MA 02215 USA
[2] Dana Farber Canc Inst, Dept Biol Chem & Mol Pharmacol, Boston, MA 02215 USA
[3] Dana Farber Canc Inst, Ctr Canc Genome Discovery, Boston, MA 02215 USA
[4] Dana Farber Canc Inst, Ludwig Ctr, Boston, MA 02215 USA
[5] Broad Inst, Cambridge, MA USA
[6] Max Planck Inst Neurol Res, Klaus Joachim Zulch Labs, Max Planck Soc, D-50931 Cologne, Germany
[7] Univ Cologne, Fac Med, D-5000 Cologne 41, Germany
[8] Univ Cologne, Dept Internal Med 1, D-5000 Cologne 41, Germany
[9] Univ Cologne, Lab Translat Canc Genom, Ctr Integrated Oncol Koln Bonn, D-5000 Cologne 41, Germany
[10] Univ Hosp Cologne, Dept Internal Med 1, Ctr Integrated Oncol Koln Bonn, Cologne, Germany
[11] Kliniken Stadt Koln gGmbH, Cologne, Germany
[12] Max Planck Gesell, Chem Genom Ctr, Dortmund, Germany
[13] Tech Univ Dortmund, Dortmund, Germany
[14] Jena Univ Hosp, Dept Hematol Oncol, Jena, Germany
[15] Haukeland Hosp, Dept Obstet & Gynecol, N-5021 Bergen, Norway
[16] Univ Bergen, Dept Clin Med, Bergen, Norway
[17] Univ Oslo, Hosp Radiumhosp, Div Surg & Canc, Oslo, Norway
[18] Univ Zurich Hosp, CH-8091 Zurich, Switzerland
[19] Univ Grenoble 1, Inst Albert Bonniot, INSERM, U823, Grenoble, France
[20] Univ Med Ctr Groningen, Dept Pulmonol, NL-9713 AV Groningen, Netherlands
[21] Univ Med Ctr Groningen, Dept Pathol, NL-9713 AV Groningen, Netherlands
[22] Univ Groningen, Groningen, Netherlands
[23] Univ Michigan, Dept Surg, Sch Med, Thorac Surg Sect, Ann Arbor, MI 48109 USA
[24] Ontario Canc Inst, Toronto, ON M4X 1K9, Canada
[25] Princess Margaret Hosp, Toronto, ON M4X 1K9, Canada
[26] H Lee Moffitt Canc Ctr & Res Inst, Dept Thorac Oncol, Tampa, FL USA
[27] H Lee Moffitt Canc Ctr & Res Inst, Dept Expt Therapeut, Tampa, FL USA
[28] Res Inst, Tampa, FL USA
关键词
DISCOIDIN DOMAIN RECEPTORS; DASATINIB; INHIBITOR; PROLIFERATION; ACTIVATION; SRC; IDENTIFICATION; EXPRESSION; GEFITINIB; APOPTOSIS;
D O I
10.1158/2159-8274.CD-11-0005
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Although genomically targeted therapies have improved outcomes for patients with lung adenocarcinoma, little is known about the genomic alterations that drive squamous cell cancer (SCC) of the lung. Sanger sequencing of the tyrosine kinome identified mutations in the DDR2 kinase gene in 3.8% of lung SCCs and cell lines. Lung SCC cell lines harboring DDR2 mutations were selectively killed by knockdown of DDR2 by RNA interference or by treatment with the multitargeted kinase inhibitor dasatinib. Tumors established from a DDR2 mutant cell line were sensitive to dasatinib in xenograft models. Expression of mutated DDR2 led to cellular transformation that was blocked by dasatinib. A patient with lung SCC that responded to dasatinib and erlotinib treatment harbored a DDR2 kinase domain mutation. These data suggest that gain-of-function mutations in DDR2 are important oncogenic events and are amenable to therapy with dasatinib. Because dasatinib is already approved for use, these findings could be used to rapidly generate clinical trials. SIGNIFICANCE: DDR2 mutations are present in 4% of lung SCCs, and DDR2 mutations are associated with sensitivity to dasatinib. These findings provide a rationale for designing clinical trials with the FDA-approved drug dasatinib in patients with lung SCCs. Cancer Discovery; 1(1); 78-89. (C) 2011 AACR.
引用
收藏
页码:78 / 89
页数:12
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