Routine molecular profiling of patients with advanced non-small-cell lung cancer: results of a 1-year nationwide programme of the French Cooperative Thoracic Intergroup (IFCT)

被引:727
作者
Barlesi, Fabrice [1 ]
Mazieres, Julien [2 ]
Merlio, Jean-Philippe [3 ,4 ]
Debieuvre, Didier [5 ]
Mosser, Jean [6 ]
Lena, Herve [7 ]
Ouafik, L'Houcine [8 ]
Besse, Benjamin [9 ,10 ]
Rouquette, Isabelle [11 ]
Westeel, Virginie [12 ]
Escande, Fabienne [13 ]
Monnet, Isabelle [14 ]
Lemoine, Antoinette [15 ]
Veillon, Remi [16 ]
Blons, Helene [17 ]
Audigier-Valette, Clarisse [18 ]
Bringuier, Pierre-Paul [19 ]
Lamy, Regine [20 ]
Beau-Faller, Michele [21 ]
Pujol, Jean-Louis [22 ]
Sabourin, Jean-Christophe [23 ]
Penault-Llorca, Frederique [24 ]
Denis, Marc G. [25 ]
Lantuejoul, Sylvie [26 ]
Morin, Franck [27 ]
Quan Tran [27 ]
Missy, Pascale [27 ]
Langlais, Alexandra [28 ]
Milleron, Bernard [29 ]
Cadranel, Jacques [29 ]
Soria, Jean-Charles [9 ,10 ]
Zalcman, Gerard [30 ]
机构
[1] Aix Marseille Univ, Ctr Invest Clin, Assistance Publ Hop Marseille, Multidisciplinary Oncol & Therapeut Innovat Dept, Marseille, France
[2] Univ Toulouse 3, Hop Larrey, Ctr Hosp Univ, F-31062 Toulouse, France
[3] Ctr Hosp Univ Bordeaux, Pole Biol & Anat Pathol, Pessac, France
[4] Univ Bordeaux, Histol & Pathol Mol Tumeurs, Bordeaux, France
[5] Hop Emile Muller, Serv Pneumol, Mulhouse, France
[6] Ctr Hosp Univ Rennes, Dept Genom & Genet Mol, Plateforme INCA, Rennes, France
[7] Ctr Hosp Univ, Hop Pontchaillou, Serv Pneumol, Rennes, France
[8] Aix Marseille Univ, Assistance Publ Hop Marseille, Serv Transfert Oncol Biol, Marseille, France
[9] Gustave Roussy, Canc Campus, Villejuif, France
[10] Univ Paris 11, Chatenay Malabry, France
[11] Inst Univ Canc Toulouse, Oncopole, Serv Anat Pathol, Toulouse, France
[12] Univ Franche Comte, EA3181, Ctr Hosp Univ Jean Minjoz, Serv Pneumol, F-25030 Besancon, France
[13] CHU Lille, Dept Biochim & Biol Mol, Ctr Biol Pathol, F-59037 Lille, France
[14] Ctr Hosp Intercommunal Creteil, Serv Pneumol & Pathol Profess, Creteil, France
[15] Univ Paris 11, Grp Hosp Hop Univ Paris Sud, AP HP, Serv Oncogenet Oncomolpath, Villejuif, France
[16] Ctr Hosp Univ Bordeaux, Serv Malad Resp, Pessac, France
[17] Univ Paris 05, INSERM, Hop Europeen Georges Pompidou, AP HP,Dept Biol, Paris, France
[18] Ctr Hosp St Musse, Serv Pneumol, Toulon, France
[19] Univ Lyon 1, Hop Edouard Herriot, Serv Anat & Cytol Pathol, Hosp Civils Lyon,Lyon Canc Res Ctr,UMR 1057,INSER, F-69365 Lyon, France
[20] Ctr Hosp Bretagne Sud, Serv Oncol Med, Lorient, France
[21] CHU Hautepierre, Lab Biochim & Biol Mol & Plate Forme Genom Canc, F-67098 Strasbourg, France
[22] CHU Montpellier, Unite Oncol Thorac, Pole Coeur Poumon, Hop Arnaud de Villeneuve, Montpellier, France
[23] Ctr Hosp Univ Rouen, Dept Anat & Cytol Pathol, Rouen, France
[24] Ctr Jean Perrin, Dept Anat & Cytol Pathol, Clermont Ferrand, France
[25] CHU Nantes, Lab Biochim, F-44035 Nantes 01, France
[26] Univ Grenoble 1, Ctr Hosp Univ A Michallon, DACP, Inst Biol & Pathol,INSERM,U823,Inst Albert Bonnio, Grenoble, France
[27] IFCT, Clin Res Unit, Paris, France
[28] IFCT, Biostat Unit, Paris, France
[29] Univ Paris 06, Sorbonne Univ, Hop Tenon, AP HP,Serv Pneumol, Paris, France
[30] Univ Caen Basse Normandie, CHU Caen, Serv Pneumol & Oncol Thorac, Ctr Rech Clin, Caen, France
关键词
GROWTH-FACTOR RECEPTOR; CLINICAL-PRACTICE; MUTATIONS; CLASSIFICATION; CHEMOTHERAPY; CRIZOTINIB; RELEVANCE; INSTITUTE; THERAPY; PROJECT;
D O I
10.1016/S0140-6736(16)00004-0
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Background The molecular profiling of patients with advanced non-small-cell lung cancer (NSCLC) for known oncogenic drivers is recommended during routine care. Nationally, however, the feasibility and effects on outcomes of this policy are unknown. We aimed to assess the characteristics, molecular profiles, and clinical outcomes of patients who were screened during a 1-year period by a nationwide programme funded by the French National Cancer Institute. Methods This study included patients with advanced NSCLC, who were routinely screened for EGFR mutations, ALK rearrangements, as well as HER2 (ERBB2), KRAS, BRAF, and PIK3CA mutations by 28 certified regional genetics centres in France. Patients were assessed consecutively during a 1-year period from April, 2012, to April, 2013. We measured the frequency of molecular alterations in the six routinely screened genes, the turnaround time in obtaining molecular results, and patients' clinical outcomes. This study is registered with ClinicalTrials.gov, number NCT01700582. Findings 18 679 molecular analyses of 17 664 patients with NSCLC were done (of patients with known data, median age was 64.5 years [range 18-98], 65% were men, 81% were smokers or former smokers, and 76% had adenocarcinoma). The median interval between the initiation of analysis and provision of the written report was 11 days (IQR 7-16). A genetic alteration was recorded in about 50% of the analyses; EGFR mutations were reported in 1947 (11%) of 17 706 analyses for which data were available, HER2 mutations in 98 (1%) of 11 723, KRAS mutations in 4894 (29%) of 17 001, BRAF mutations in 262 (2%) of 13 906, and PIK3CA mutations in 252 (2%) of 10 678; ALK rearrangements were reported in 388 (5%) of 8134 analyses. The median duration of follow-up at the time of analysis was 24.9 months (95% CI 24.8-25.0). The presence of a genetic alteration affected first-line treatment for 4176 (51%) of 8147 patients and was associated with a significant improvement in the proportion of patients achieving an overall response in first-line treatment (37% [95% CI 34.7-38.2] for presence of a genetic alteration vs 33% [29.5-35.6] for absence of a genetic alteration; p=0.03) and in second-line treatment (17% [15.0-18.8] vs 9% [6.7-11.9]; p<0.0001). Presence of a genetic alteration was also associated with improved first-line progression-free survival (10.0 months [95% CI 9.2-10.7] vs 7.1 months [6.1-7.9]; p<0.0001) and overall survival (16.5 months [15.0-18.3] vs 11.8 months [10.1-13.5]; p<0.0001) compared with absence of a genetic alteration. Interpretation Routine nationwide molecular profiling of patients with advanced NSCLC is feasible. The frequency of genetic alterations, acceptable turnaround times in obtaining analysis results, and the clinical advantage provided by detection of a genetic alteration suggest that this policy provides a clinical benefit.
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收藏
页码:1415 / 1426
页数:12
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