DNA methylation of multiple genes in gastric carcinoma: Association with histological type and CpG island methylator phenotype

Oue, Naohide; Oshimo, Yasuhiro; Nakayama, Hirofumi; Ito, Reiko; Yoshida, Kazuhiro; Matsusaki, Keisuke; Yasui, Wataru

doi:10.1111/j.1349-7006.2003.tb01373.x

Cited by 95 publications

(82 citation statements)

References 26 publications

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“…Using different DNA methylation markers and different methodology, CpG island methylator phenotype was found to be associated with 'diffuse' histology in some reports 33,38 but not in others. 39,40 These controversial findings are most likely due to the use of differing DNA methylation marker panels as well as methods of analysis. In the present study, we analyzed 27 DNA methylation markers using the MethyLight technology and diffuse-type GC showed a significantly higher frequency of CpG island hypermethylation than intestinaltype GC, although the number of cases was limited.…”

Section: Methylation In Gc Was Revealed For the First Time In Thismentioning

confidence: 99%

DNA methylation profiles of gastric carcinoma characterized by quantitative DNA methylation analysis

Kang

Lee

Cho

et al. 2008

Laboratory Investigation

153

107

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Transcriptional silencing by CpG island hypermethylation is a potential mechanism for the inactivation of tumor-related genes. Virtually, all types of human cancers show CpG island hypermethylation, and gastric carcinoma (GC) is one of the tumors with a high frequency of aberrant CpG island hypermethylation. In this study, we prescreened DNA methylation of 170 CpG island loci in a training set of 8 paired GC and GC-associated non-neoplastic mucosae (GCN) using MethyLight technology and selected 27 DNA methylation markers showing higher methylation frequency or level in GC than in GCN. These markers were then analyzed in a tester set of 25 paired GC and GCN and 27 chronic gastritis (CG) from non-cancer patients to generate their DNA methylation profiles. We identified 17 novel methylation markers in GC, including SFRP4, SEZ6L, TWIST1, BCL2, KL, TERT, SCGB3A1, IGF2, GRIN2B, SFRP5, DLEC1, HOXA1, CYP1B1, SMAD9, MT1G, NR3C1, and HOXA10. Of the 27 selected CpG island loci, 23 were methylated in GC, GCN, and CG and the remainder four loci (DLEC1, CHFR, CYP1B1, and NR3C1) were only methylated in GC. We found that the number of methylated loci was significantly higher in GC than in GCN or CG and that Helicobacter pylori infection was strongly associated with aberrant CpG island hypermethylation in CG. Hypermethylation was more prevalent in Epstein-Barr virus (EBV)-positive GC than in EBV-negative GC and in diffuse-type GC than in intestinal-type GC. Through our large-scale screening of 170 CpG island loci, we found 17 new DNA methylation markers of GC, which may serve as useful markers that may identify a distinct subset of GC.

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Section: Methylation In Gc Was Revealed For the First Time In Thismentioning

confidence: 99%

DNA methylation profiles of gastric carcinoma characterized by quantitative DNA methylation analysis

Kang

Lee

Cho

et al. 2008

Laboratory Investigation

153

107

View full text Add to dashboard Cite

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“…13 The presence or absence of CIMP and DNA methylation of 5 genes (hMLH1, MGMT, p16 INK4a , CDH1, and RAR-beta) was determined previously. 15 …”

Section: Bisulfite Polymerase Chain Reaction (Pcr) and Methylation-spmentioning

confidence: 99%

“…13 Originally CIMP-positive GC was defined as a tumor with methylation at more than 3 loci methylated in tumors (MINT: MINT1, MINT2, MINT12, MINT25, and MINT31). 13 CIMP-positive GCs also tend to show DNA methylation of the p16 INK4a , 13 hMLH1, 15 and RIZ1 genes, 16 suggesting that CIMP is an important pathway involved in stomach carcinogenesis. However, limited numbers of genes have been shown to be associated with CIMP-positive GC, and the role of CIMP has not been clarified in detail.…”

mentioning

confidence: 99%

Accumulation of DNA methylation is associated with tumor stage in gastric cancer

Oue

Mitani

Motoshita

et al. 2006

Cancer

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129

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We present a methodological framework for estimating the degree of mixing between successive miscible fluids pumped along a near‐horizontal pipe. Either or both of the fluids can be non‐Newtonian, of Herschel–Bulkley type. Overall it is considered that the objective is to minimise mixing. In laminar regimes our estimates are based on front velocity of the leading displacement front. In turbulent regimes the spreading mechanism is dispersion. In addition to the estimates of mixing volumes/lengths, we also predict a minimal flow rate necessary in order to achieve a successful displacement of the residual fluid. © 2013 Canadian Society for Chemical Engineering

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“…Furthermore, concurrent promoter hypermethylation of multiple genes, which is termed descriptively as the 'CpG island methylator phenotype' (CIMP), was also described in gastric cancers. 7 Although, the epigenetic changes have been accepted as an important mechanism underlying tumor onset and progression, there are limited data related to factors inducing methylation. Recent studies have indicated the existence of a mechanistic linkage between DNA methylation and infectious agents.…”

mentioning

confidence: 99%

The presence of JC virus in gastric carcinomas correlates with patient's age, intestinal histological type and aberrant methylation of tumor suppressor genes

et al. 2010

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JC virus (JCV) is a neurotropic polyomavirus and the causative agent of progressive multifocal leukoencephalopathy. A role for JCV in gastrointestinal malignancies has been recently suggested. This study was carried out to determine the prevalence of polyomaviruses including JCV, BKV and SV40 in gastric cancers in Tunisia and to determine the clinicopathological characteristics of virus-associated gastric carcinomas. The presence of polyomaviruses DNA sequences was surveyed in 61 cases of primary gastric carcinomas and in 53 paired non-tumor gastric mucosa by PCR. Findings were correlated to clinicopathological parameters, p53 expression and methylation status of 11 tumor-related genes. Using PCR assays, JCV T-antigen sequence was more frequently detected in gastric carcinomas than in non-tumor gastric mucosa (26 vs 6%, P ¼ 0.03), while those of SV40 and BKV were not detected in any cases. Correlation analysis showed that JCV had higher frequency in patients older than 55 years (P ¼ 0.034) and in the intestinal histological type (P ¼ 0.04). With regard to methylation status, P16 and P14 showed significantly higher methylation frequencies in JCV-positive gastric carcinomas than in JCV-negative cases (P ¼ 0.007 and P ¼ 0.003, respectively). Moreover, the mean of the methylation index was significantly higher in JCV-positive than in JCV-negative cases (P ¼ 0.024). In multivariate logistic regression analysis, age of patients and the methylation index are only the two independent factors associated with JCV infection. Kaplan-Meier survival analysis showed a trend toward better survival for JCV-associated gastric carcinomas patients (log-rank, P ¼ 0.11). Our study suggests a role of JCV as cofactor in the pathogenesis of the intestinal type of gastric carcinomas in older persons.

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DNA methylation of multiple genes in gastric carcinoma: Association with histological type and CpG island methylator phenotype

Cited by 95 publications

References 26 publications

DNA methylation profiles of gastric carcinoma characterized by quantitative DNA methylation analysis

DNA methylation profiles of gastric carcinoma characterized by quantitative DNA methylation analysis

Accumulation of DNA methylation is associated with tumor stage in gastric cancer

The presence of JC virus in gastric carcinomas correlates with patient's age, intestinal histological type and aberrant methylation of tumor suppressor genes

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