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Oncogene Mutations in Colorectal Polyps Identified in the Norwegian Colorectal Cancer Prevention (NORCCAP) Screening Study
Author(s) -
Jon A. Lorentzen,
Krzysztof Grzyb,
Paula M. De Angelis,
Geir Hoff,
Tor J. Eide,
Per Arne Andresen
Publication year - 2016
Publication title -
clinical medicine insights pathology
Language(s) - English
Resource type - Journals
ISSN - 1179-5557
DOI - 10.4137/cpath.s40143
Subject(s) - kras , colorectal cancer , medicine , carcinogenesis , cancer , mutation , exon , oncogene , population , oncology , cancer research , biology , genetics , gene , environmental health , cell cycle
Data are limited on oncogene mutation frequencies in polyps from principally asymptomatic participants of population-based colorectal cancer screening studies. In this study, DNA from 204 polyps, 5 mm or larger, were collected from 176 participants of the NORCCAP screening study and analyzed for mutations in KRAS, BRAF, and PIK3CA including the rarely studied KRAS exons 3 and 4 mutations. KRAS mutations were identified in 23.0% of the lesions and were significantly associated with tubulovillous adenomas and large size. A significantly higher frequency of KRAS mutations in females was associated with mutations in codon 12. The KRAS exon 3 and 4 mutations constituted 23.4% of the KRAS positive lesions, which is a larger proportion compared to previous observations in colorectal cancer. BRAF mutations were identified in 11.3% and were associated with serrated polyps. None of the individuals were diagnosed with de novo or recurrent colorectal cancer during the follow-up time (median 11.2 years). Revealing differences in mutation-spectra according to gender and stages in tumorigenesis might be important for optimal use of oncogenes as therapeutic targets and biomarkers.

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