Literature DB >> 21239505

KRAS mutation is associated with lung metastasis in patients with curatively resected colorectal cancer.

Jeanne Tie1, Lara Lipton, Jayesh Desai, Peter Gibbs, Robert N Jorissen, Michael Christie, Katharine J Drummond, Benjamin N J Thomson, Valery Usatoff, Peter M Evans, Adrian W Pick, Simon Knight, Peter W G Carne, Roger Berry, Adrian Polglase, Paul McMurrick, Qi Zhao, Dana Busam, Robert L Strausberg, Enric Domingo, Ian P M Tomlinson, Rachel Midgley, David Kerr, Oliver M Sieber.   

Abstract

PURPOSE: Oncogene mutations contribute to colorectal cancer development. We searched for differences in oncogene mutation profiles between colorectal cancer metastases from different sites and evaluated these as markers for site of relapse. EXPERIMENTAL
DESIGN: One hundred colorectal cancer metastases were screened for mutations in 19 oncogenes, and further 61 metastases and 87 matched primary cancers were analyzed for genes with identified mutations. Mutation prevalence was compared between (a) metastases from liver (n = 65), lung (n = 50), and brain (n = 46), (b) metastases and matched primary cancers, and (c) metastases and an independent cohort of primary cancers (n = 604). Mutations differing between metastasis sites were evaluated as markers for site of relapse in 859 patients from the VICTOR trial.
RESULTS: In colorectal cancer metastases, mutations were detected in 4 of 19 oncogenes: BRAF (3.1%), KRAS (48.4%), NRAS (6.2%), and PIK3CA (16.1%). KRAS mutation prevalence was significantly higher in lung (62.0%) and brain (56.5%) than in liver metastases (32.3%; P = 0.003). Mutation status was highly concordant between primary cancer and metastasis from the same individual. Compared with independent primary cancers, KRAS mutations were more common in lung and brain metastases (P < 0.005), but similar in liver metastases. Correspondingly, KRAS mutation was associated with lung relapse (HR = 2.1; 95% CI, 1.2 to 3.5, P = 0.007) but not liver relapse in patients from the VICTOR trial.
CONCLUSIONS: KRAS mutation seems to be associated with metastasis in specific sites, lung and brain, in colorectal cancer patients. Our data highlight the potential of somatic mutations for informing surveillance strategies. ©2011 AACR.

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Year:  2011        PMID: 21239505     DOI: 10.1158/1078-0432.CCR-10-1720

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  86 in total

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4.  RAS mutation status predicts survival and patterns of recurrence in patients undergoing hepatectomy for colorectal liver metastases.

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5.  Mutational analysis and clinical correlation of metastatic colorectal cancer.

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Journal:  Cancer       Date:  2014-02-05       Impact factor: 6.860

6.  Integration of microenvironmental and stress signaling antagonizes colorectal cancer progression.

Authors:  Nina Linde; Maria Soledad Sosa; Julio A Aguirre-Ghiso
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7.  Significance of RAS mutations in pulmonary metastases of patients with colorectal cancer.

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Journal:  Int J Clin Oncol       Date:  2019-11-26       Impact factor: 3.402

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9.  RAS mutations affect pattern of metastatic spread and increase propensity for brain metastasis in colorectal cancer.

Authors:  Rona Yaeger; Elizabeth Cowell; Joanne F Chou; Alexandra N Gewirtz; Laetitia Borsu; Efsevia Vakiani; David B Solit; Neal Rosen; Marinela Capanu; Marc Ladanyi; Nancy Kemeny
Journal:  Cancer       Date:  2014-12-09       Impact factor: 6.860

Review 10.  Management of resectable colorectal lung metastases.

Authors:  Sing Yu Moorcraft; George Ladas; Anne Bowcock; Ian Chau
Journal:  Clin Exp Metastasis       Date:  2015-12-10       Impact factor: 5.150

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