Haploinsufficiency by minute MutL homolog 1 promoter DNA methylation may represent unique phenotypes of microsatellite instability-gastric carcinogenesis

Harada, Hiroki and Nie, Yusuke and Araki, Ippeita and Soeno, Takafumi and Chuman, Motohiro and Washio, Marie and Sakuraya, Mikiko and Ushiku, Hideki and Niihara, Masahiro and Hosoda, Kei and Kumamoto, Yusuke and Naitoh, Takeshi and Sangai, Takafumi and Hiki, Naoki and Yamashita, Keishi and Suzuki, Hiromu (2021) Haploinsufficiency by minute MutL homolog 1 promoter DNA methylation may represent unique phenotypes of microsatellite instability-gastric carcinogenesis. PLOS ONE, 16 (12). e0260303. ISSN 1932-6203

[thumbnail of journal.pone.0260303.pdf] Text
journal.pone.0260303.pdf - Published Version

Download (2MB)

Abstract

Promoter DNA methylation of MutL homolog 1 (MLH1) is considered to play a causative role in microsatellite instability (MSI) carcinogenesis in primary gastric cancer, and a high MSI status is associated with treatment sensitivity to human cancers. Nevertheless, clinicopathological analysis is defective for MLH1 methylation status in a quantitative manner. We newly developed quantitative methylation specific PCR using a TaqMan probe and applied it to 138 patients with primary gastric cancer who underwent gastrectomy in addition to basic molecular features such as MSI, Epstein Barr virus, and other DNA methylation status. (1) In primary gastric cancer, median methylation value was 0.055, ranging from 0 to 124.3. First, MLH1 hypermethylation was strongly correlated with MSI-High/MSI-Low status and suppressed immunostaining (P < 0.0001). (2) The MLH1 hypermethylation was associated with advanced age (P = 0.0048), antral location (P = 0.0486), synchronous multiple gastric cancer (P = 0.0001), and differentiated histology (P = 0.028). (3) Log-rank plot analysis identified the most relevant cut-off value (0.23) to reflect gentle phenotypes in MLH1 hypermethylation cases (P = 0.0019), especially in advanced gastric cancer (P = 0.0132), which are designated as haploinsufficiency of MSI (MSI-haplo) phenotype in this study. (4) In synchronous multiple gastric cancer, MLH1 hypermethylation was not necessarily confirmed as field cancerization. (5) MSI-haplo defined by MLH1 methylation status represented distinct prognostic phenotype even after molecular classifications. MLH1 hypermethylation designated as MSI-haplo may represent unique prognostic phenotype during gastric carcinogenesis.

Item Type: Article
Subjects: Scholar Eprints > Biological Science
Depositing User: Managing Editor
Date Deposited: 26 Dec 2022 05:08
Last Modified: 07 Sep 2024 10:55
URI: http://repository.stmscientificarchives.com/id/eprint/475

Actions (login required)

View Item
View Item