Aberrant CpG Island Hypermethylation of Chronic Gastritis, in Relation to Aging, Gender, Intestinal Metaplasia, and Chronic Inflammation

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Aberrant CpG Island Hypermethylation of Chronic Gastritis, in Relation to Aging, Gender, Intestinal Metaplasia, and Chronic Inflammation

Gyeong Hoon Kang^*, Hyeon Joo Lee^*, Kyu Sang Hwang^*, Sun Lee, Jae-Hoon Kim^* and Jung-Sun Kim

From the Department of Pathology and Cancer Research Institute,^* Seoul National University College of Medicine, Seoul; the Department of Pathology, National Cancer Center, Goyang, Gyeonggi; and the Department of Diagnostic Pathology, University of Ulsan College of Medicine, Seoul, Korea

Aberrant hypermethylation of promoter CpG islands is an importantmechanism for the inactivation of tumor suppressor genes. CpGisland hypermethylation occurs in relation to tumorigenesisor aging. Gastric cancer is one of the tumors with a high levelof aberrant CpG island methylation. However, the data on themethylation status of normal gastric mucosa has been very limited.The present study attempted to compare the methylation statusof nonneoplastic gastric mucosa, using clinicopathological parameters,including age, gender, Helicobacter pylori (H. pylori), acuteand chronic inflammation, and intestinal metaplasia. Two hundredsixty-eight nonneoplastic gastric mucosa samples were studiedfor the methylation status of 11 genes (COX-2, DAP-kinase, E-cadherin,GSTP1, MGMT, hMLH1, p14, p16, THBS1, TIMP3, and RASSF1A), usingmethylation-specific PCR. CpG island hypermethylation was foundin 53.7, 41, 37.7, 23.1, 18.7, 10.9, 10, 4.1, 3.4, 1.7, 0.4%for DAP-kinase, E-cadherin, THBS1, TIMP3, p14, MGMT, p16, COX-2,GSTP1, hMLH1 and RASSF1A, respectively. Five genes (DAP-kinase,E-cadherin, p14, THBS1, and TIMP-3) showed a general progressiveincrease in the methylation frequency as a function of aging,whereas the other genes (COX-2, GSTP1, MGMT, hMLH1, p16, andRASSF1A) were rarely methylated. Male patients showed highernumbers of methylated genes than females (3.2 vs. 2.1, respectively,P = 0.002). Gastritis samples with marked intestinal metaplasia,showed higher numbers of genes methylated than those without(3.7 vs. 2.6, respectively, P = 0.021). Gastritis samples withmarked infiltration of mononuclear cells displayed higher numbersof genes methylated than those with mild or moderate infiltrationof mononuclear cells (3.4 vs. 2.5 or 2.5, respectively, P <0.05). Our results demonstrated that many genes are methylatedin the stomach as a function of age, and suggested that malegender, intestinal metaplasia, and chronic inflammation areclosely associated with increased methylation in nonneoplasticgastric mucosa samples.

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