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Erschienen in: Gastric Cancer 6/2019

12.03.2019 | Original Article

DNA methylation genome-wide analysis in remnant and primary gastric cancers

verfasst von: Kiichi Sugimoto, Tomoaki Ito, Alicia Hulbert, Chen Chen, Hajime Orita, Masahiro Maeda, Hiroshi Moro, Takeo Fukagawa, Toshikazu Ushijima, Hitoshi Katai, Ryo Wada, Koichi Sato, Kazuhiro Sakamoto, Wayne Yu, Michael Considine, Leslie Cope, Malcolm V. Brock

Erschienen in: Gastric Cancer | Ausgabe 6/2019

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Abstract

Background

Although primary (PGC) and remnant gastric cancers (RGC) both originate from the same gastrointestinal organ, they have very distinct clinicopathological behaviors. We hypothesized that there would be distinct differences in DNA methylation patterns that would occur during carcinogenesis of RGC and PGC, and that the differences in methylation patterns may help identify the primary factor contributing to chronic inflammation in patients with RGC.

Methods

We investigated the genome-wide DNA methylation patterns of PGC and RGC tissues from 48 patients using the Infinium HumanMethylation450 Beadchip assay. The results were validated by quantitative methylation-specific PCR (qMSP) in separate, independent cohorts.

Results

We found that in our training cohort of 48 patients, the most variable genes from the gastric cancer tissues identified by the Infinium HumanMethylation450 Beadchip clustered the resultant heatmap into high and low methylation groups. On multivariate analysis, PGCs contributed significantly to the high methylation group (p = 0.004, OR 12.33), which suggested that the promoter methylation status in PGC is higher than that in RGC. Supporting this conclusion was the finding that in a separate qMSP analysis in a test cohort, the EPB41L3 gene, chosen because of its high β value on microarray analysis in the gastric cancer tissues, had significantly higher DNA promoter methylation in cancer tissues in the validation PGC tissues than in RGC.

Conclusions

This study demonstrated that promoter methylation status in PGC is higher than in RGC. This result may reflect the effects of the absence of Helicobacter pylori on the reduced DNA methylation in the remnant stomach.
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Metadaten
Titel
DNA methylation genome-wide analysis in remnant and primary gastric cancers
verfasst von
Kiichi Sugimoto
Tomoaki Ito
Alicia Hulbert
Chen Chen
Hajime Orita
Masahiro Maeda
Hiroshi Moro
Takeo Fukagawa
Toshikazu Ushijima
Hitoshi Katai
Ryo Wada
Koichi Sato
Kazuhiro Sakamoto
Wayne Yu
Michael Considine
Leslie Cope
Malcolm V. Brock
Publikationsdatum
12.03.2019
Verlag
Springer Singapore
Erschienen in
Gastric Cancer / Ausgabe 6/2019
Print ISSN: 1436-3291
Elektronische ISSN: 1436-3305
DOI
https://doi.org/10.1007/s10120-019-00949-5

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