DNA methylation epigenotype and clinical features of NRAS‐mutation(+) colorectal cancer

DNA methylation epigenotype and clinical features of NRAS‐mutation(+) colorectal cancer

Sporadic colorectal cancer (CRC) is classified into several molecular subtypes. We previously established two groups of DNA methylation markers through genome‐wide DNA methylation analysis to classify CRC into distinct subgroups: high‐, intermediate‐, and low‐methylation epigenotypes (HME, IME, and...

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Veröffentlicht in:Cancer medicine (Malden, MA) MA), 2017-05, Vol.6 (5), p.1023-1035
Hauptverfasser: Takane, Kiyoko, Akagi, Kiwamu, Fukuyo, Masaki, Yagi, Koichi, Takayama, Tadatoshi, Kaneda, Atsushi
Format: Artikel
Sprache:eng
Schlagworte:
Age Factors
Aged
Aged, 80 and over
BRAF mutation
Clinical Cancer Research
Colorectal cancer
Colorectal carcinoma
Colorectal Neoplasms - genetics
Colorectal Neoplasms - pathology
CpG Islands
Deoxyribonucleic acid
DNA
DNA Methylation
Epigenesis, Genetic
Female
Genes
Genomes
GTP Phosphohydrolases - genetics
Humans
KRAS mutation
Male
Membrane Proteins - genetics
Middle Aged
Mutation
Neoplasm Invasiveness
NRAS mutation
Original Research
Phenotypes
Prognosis
Proto-Oncogene Proteins p21(ras) - genetics
Sequence Analysis, DNA
Survival Analysis
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Zusammenfassung:Sporadic colorectal cancer (CRC) is classified into several molecular subtypes. We previously established two groups of DNA methylation markers through genome‐wide DNA methylation analysis to classify CRC into distinct subgroups: high‐, intermediate‐, and low‐methylation epigenotypes (HME, IME, and LME, respectively). HME CRC, also called CpG island methylator phenotype (CIMP)‐high CRC, shows methylation of both Group 1 markers (CIMP markers) and Group 2 markers, while IME/CIMP‐low CRC shows methylation of Group 2, but not of Group 1 markers, and LME CRC shows no methylation of either Group 1 or Group 2 markers. While BRAF‐ and KRAS‐mutation(+) CRC strongly correlated with HME and IME, respectively, clinicopathological features of NRAS‐mutation(+) CRC, including association with DNA methylation, remain unclear. To characterize NRAS‐mutation(+) CRC, the methylation levels of 19 methylation marker genes (6 Group 1 and 13 Group 2) were analyzed in 61 NRAS‐mutation(+) and 144 NRAS‐mutation(−) CRC cases by pyrosequencing, and their correlation with clinicopathological features was investigated. Different from KRAS‐mutation(+) CRC, NRAS‐mutation(+) CRC significantly correlated with LME. NRAS‐mutation(+) CRC showed significantly better prognosis than KRAS‐mutation(+) CRC (P = 3 × 10−4). NRAS‐mutation(+) CRC preferentially occurred in elder patients (P = 0.02) and at the distal colon (P = 0.006), showed significantly less lymph vessel invasion (P = 0.002), and correlated with LME (P = 8 × 10−5). DNA methylation significantly accumulated at the proximal colon. NRAS‐mutation(+) CRC may constitute a different subgroup from KRAS‐mutation(+) CRC, showing significant correlation with LME, older age, distal colon, and relatively better prognosis. Genetic and epigenetic analyses of colorectal cancer (CRC) were conducted to clarify molecular and clinicopathological features of NRAS‐mutation(+) CRC compared to KRAS‐mutation(+) and other subgroups of CRC. NRAS‐mutation(+) CRC presented a low‐methylation epigenotype, occurred in elder patients and at the distal colon, and showed relatively better prognosis
ISSN:2045-7634
2045-7634
DOI:10.1002/cam4.1061