Prognostic significance of K-Ras mutation rate in metastatic colorectal cancer patients

被引:29
作者
Vincenzi, Bruno [1 ]
Cremolini, Chiara [2 ]
Sartore-Bianchi, Andrea [3 ]
Russo, Antonio [4 ]
Mannavola, Francesco [5 ]
Perrone, Giuseppe [6 ]
Pantano, Francesco [1 ]
Loupakis, Fotios [2 ]
Rossini, Daniele [2 ]
Ongaro, Elena [7 ]
Bonazzina, Erica [3 ]
Dell'Aquila, Emanuela [1 ]
Imperatori, Marco [1 ]
Zoccoli, Alice [1 ]
Bronte, Giuseppe [4 ]
De Maglio, Giovanna [7 ]
Fontanini, Gabriella [8 ]
Natoli, Clara [9 ]
Falcone, Alfredo [2 ]
Santini, Daniele [1 ]
Onetti-Muda, Andrea [6 ]
Siena, Salvatore [3 ]
Tonini, Giuseppe [1 ]
Aprile, Giuseppe [7 ]
机构
[1] Campus Biomed Univ Rome, Dept Med Oncol, Rome, Italy
[2] Azienda Osped Univ Pisana, Ist Toscano Tumori, Pisa, Italy
[3] Osped Niguarda Ca Granda, Niguarda Canc Ctr, Milan, Italy
[4] Univ Palermo, Dept Surg Oncol & Oral Sci, Sect Med Oncol, Palermo, Italy
[5] Univ Cattolica Sacro Cuore, Rome, Italy
[6] Campus Biomed Univ Rome, Dept Anat Pathol, Rome, Italy
[7] Azienda Osped Univ, Dept Med Oncol, Udine, Italy
[8] Univ Pisa, Dipartimento Patol Chirurg Med Mol & Area Crit, Pisa, Italy
[9] Univ G DAnnunzio, Dept Med Oral & Biotechnol Sci, Chieti, Italy
来源
ONCOTARGET | 2015年 / 6卷 / 31期
关键词
K-Ras; mutation rate; colorectal cancer; bevacizumab; prognosis; WILD-TYPE; KRAS; CETUXIMAB; PANITUMUMAB; BRAF; METAANALYSIS; CONCORDANCE; IRINOTECAN; RESISTANCE; SURVIVAL;
D O I
10.18632/oncotarget.5231
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Introduction: Activating mutations of K-Ras gene have a well-established role as predictors of resistance to anti-EGFR monoclonal antibodies in metastatic colorectal cancer (mCRC) patients. Their prognostic value is controversial, and no data regarding the prognostic value of mutation rate, defined as the percentage of mutated alleles/tumor sample, are available. We aimed to evaluate the prognostic value of K-Ras mutation rate in a homogenous cohort of mCRC patients receiving first-line doublet plus bevacizumab. Patients and Methods: This retrospective study enrolled 397 K-Ras mutant mCRC patients from 6 Italian centers, and 263 patients were fully evaluable for our analysis. K-Ras mutation rate was assessed by pyrosequencing. Patients with less than 60% of cancer cells in tumor tissue were excluded. No patients received anti-EGFR containing anticancer therapy, at any time. Median mutation rate was 40% and was adopted as cut-off. The primary and secondary endpoints were PFS and OS respectively. Results: At univariate analysis, K-Ras mutation rate higher than 40% was significantly associated with lower PFS (7.3 vs 9.1 months; P < 0.0001) and OS (21 vs 31 months; P = 0.004). A multivariate model adjusted for age at diagnosis, site of origin of tumor tissue (primary vs metastases), referral center, number of metastatic sites, and first-line chemotherapy backbone, showed that K-Ras mutation rate remained a significant predictor of PFS and OS in the whole population. Discussion: Our data demonstrate an association between K-Ras mutation rate and prognosis in mCRC patients treated with bevacizumab-containing first-line therapy. These data deserve to be verified in an independent validation set.
引用
收藏
页码:31604 / 31612
页数:9
相关论文
共 28 条
[1]   Blocking oncogenic Ras signaling for cancer therapy [J].
Adjei, AA .
JNCI-JOURNAL OF THE NATIONAL CANCER INSTITUTE, 2001, 93 (14) :1062-1074
[2]   Wild-type KRAS is required for panitumumab efficacy in patients with metastatic colorectal cancer [J].
Amado, Rafael G. ;
Wolf, Michael ;
Peeters, Marc ;
Van Cutsem, Eric ;
Siena, Salvatore ;
Freeman, Daniel J. ;
Juan, Todd ;
Sikorski, Robert ;
Suggs, Sid ;
Radinsky, Robert ;
Patterson, Scott D. ;
Chang, David D. .
JOURNAL OF CLINICAL ONCOLOGY, 2008, 26 (10) :1626-1634
[3]   Kirsten ras mutations in patients with colorectal cancer:: the 'RASCAL II' study [J].
Andreyev, HJN ;
Norman, AR ;
Cunningham, D ;
Oates, J ;
Dix, BR ;
Iacopetta, BJ ;
Young, J ;
Walsh, T ;
Ward, R ;
Hawkins, N ;
Beranek, M ;
Jandik, P ;
Benamouzig, R ;
Jullian, E ;
Laurent-Puig, P ;
Olschwang, S ;
Muller, O ;
Hoffmann, I ;
Rabes, HM ;
Zietz, C ;
Troungos, C ;
Valavanis, C ;
Yuen, ST ;
Ho, JWC ;
Croke, CT ;
O'Donoghue, DP ;
Giaretti, W ;
Rapallo, A ;
Russo, A ;
Bazan, V ;
Tanaka, M ;
Omura, K ;
Azuma, T ;
Ohkusa, T ;
Fujimori, T ;
Ono, Y ;
Pauly, M ;
Faber, C ;
Glaesener, R ;
de Goeij, AFPM ;
Arends, JW ;
Andersen, SN ;
Lövig, T ;
Breivik, J ;
Gaudernack, G ;
Clausen, OPF ;
De Angelis, P ;
Meling, GI ;
Rognum, TO ;
Smith, R .
BRITISH JOURNAL OF CANCER, 2001, 85 (05) :692-696
[4]   Comparative sequencing analysis reveals high genomic concordance between matched primary and metastatic colorectal cancer lesions [J].
Brannon, A. Rose ;
Vakiani, Efsevia ;
Sylvester, Brooke E. ;
Scott, Sasinya N. ;
McDermott, Gregory ;
Shah, Ronak H. ;
Kania, Krishan ;
Viale, Agnes ;
Oschwald, Dayna M. ;
Vacic, Vladimir ;
Emde, Anne-Katrin ;
Cercek, Andrea ;
Yaeger, Rona ;
Kemeny, Nancy E. ;
Saltz, Leonard B. ;
Shia, Jinru ;
D'Angelica, Michael I. ;
Weiser, Martin R. ;
Solit, David B. ;
Berger, Michael F. .
GENOME BIOLOGY, 2014, 15 (08)
[5]   HeR2 Signaling and Resistance to the Anti-EGFR Monoclonal Antibody Cetuximab: A Further Step toward Personalized Medicine for Patients with Colorectal Cancer [J].
Ciardiello, Fortunato ;
Normanno, Nicola .
CANCER DISCOVERY, 2011, 1 (06) :472-474
[6]   Effects of KRAS, BRAF, NRAS, and PIK3CA mutations on the efficacy of cetuximab plus chemotherapy in chemotherapy-refractory metastatic colorectal cancer: a retrospective consortium analysis [J].
De Roock, Wendy ;
Claes, Bart ;
Bernasconi, David ;
De Schutter, Jef ;
Biesmans, Bart ;
Fountzilas, George ;
Kalogeras, Konstantine T. ;
Kotoula, Vassiliki ;
Papamichael, Demetris ;
Laurent-Puig, Pierre ;
Penault-Llorca, Frederique ;
Rougier, Philippe ;
Vincenzi, Bruno ;
Santini, Daniele ;
Tonini, Giuseppe ;
Cappuzzo, Federico ;
Frattini, Milo ;
Molinari, Francesca ;
Saletti, Piercarlo ;
De Dosso, Sara ;
Martini, Miriam ;
Bardelli, Alberto ;
Siena, Salvatore ;
Sartore-Bianchi, Andrea ;
Tabernero, Josep ;
Macarulla, Teresa ;
Di Fiore, Frederic ;
Gangloff, Alice Oden ;
Ciardiello, Fortunato ;
Pfeiffer, Per ;
Qvortrup, Camilla ;
Hansen, Tine Plato ;
Van Cutsem, Eric ;
Piessevaux, Hubert ;
Lambrechts, Diether ;
Delorenzi, Mauro ;
Tejpar, Sabine .
LANCET ONCOLOGY, 2010, 11 (08) :753-762
[7]   Wild-Type BRAF Is Required for Response to Panitumumab or Cetuximab in Metastatic Colorectal Cancer [J].
Di Nicolantonio, Federica ;
Martini, Miriam ;
Molinari, Francesca ;
Sartore-Bianchi, Andrea ;
Arena, Sabrina ;
Saletti, Piercarlo ;
De Dosso, Sara ;
Mazzucchelli, Luca ;
Frattini, Milo ;
Siena, Salvatore ;
Bardelli, Alberto .
JOURNAL OF CLINICAL ONCOLOGY, 2008, 26 (35) :5705-5712
[8]   Panitumumab-FOLFOX4 Treatment and RAS Mutations in Colorectal Cancer [J].
Douillard, Jean-Yves ;
Oliner, Kelly S. ;
Siena, Salvatore ;
Tabernero, Josep ;
Burkes, Ronald ;
Barugel, Mario ;
Humblet, Yves ;
Bodoky, Gyorgy ;
Cunningham, David ;
Jassem, Jacek ;
Rivera, Fernando ;
Kocakova, Ilona ;
Ruff, Paul ;
Blasinska-Morawiec, Maria ;
Smakal, Martin ;
Canon, Jean Luc ;
Rother, Mark ;
Williams, Richard ;
Rong, Alan ;
Wiezorek, Jeffrey ;
Sidhu, Roger ;
Patterson, Scott D. .
NEW ENGLAND JOURNAL OF MEDICINE, 2013, 369 (11) :1023-1034
[9]  
Dupont Jensen J, 2014, J CLIN ONCOL S3, V32
[10]   COSMIC 2005 [J].
Forbes, S ;
Clements, J ;
Dawson, E ;
Bamford, S ;
Webb, T ;
Dogan, A ;
Flanagan, A ;
Teague, J ;
Wooster, R ;
Futreal, PA ;
Stratton, MR .
BRITISH JOURNAL OF CANCER, 2006, 94 (02) :318-322
123