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DNA Methylation as Surrogate Marker For Gastric Cancer. | LitMetric

DNA Methylation as Surrogate Marker For Gastric Cancer.

J Cancer Prev

Microbiology, College of Medicine, The Catholic University of Korea, Seoul, Korea.

Published: September 2015

AI Article Synopsis

  • Stomach cancer is still very common in East Asia, but predicting it is challenging due to a lack of biomarkers, with Helicobacter pylori being a major risk factor that often goes unrecognized before diagnosis.
  • The study suggests a new approach using DNA methylation markers identified through endoscopic biopsies, focusing on specific methylation changes linked to H. pylori and age.
  • These methylation patterns could help in developing personalized screening intervals for those at high risk, improving prognosis and management for patients with early-stage stomach cancer.

Article Abstract

Stomach cancer remains, stubbornly, highly prevalent in East Asia. Still, stomach cancer has few biomarkers by which it can be predicted. Helicobacter pylori infection, a known carcinogen of stomach cancer, usually goes undetected prior to cancer diagnosis, due to the poor mucosal environments that its related gastric atrophy causes. We propose, herein, an endoscopic-biopsy-based cancer-predicting DNA methylation marker. We semi-quantitatively examined the methylation-variable sites near the CpG-island margins by radioisotope-labeling methylation-specific polymerase chain reaction in association with H. pylori, which increases age-related over-methylation in CpG islands of gastric mucosa. These age-related methylation patterns of the transitional-CpG sites are proposed as useful surrogate markers for stomach cancer. It would be helpful for setting the optimal screening interval for high-risk subjects as well as for estimating the prognosis and the predictability for recurrence of early gastric cancer in patients having undergone endoscopic submucosal dissection. New screening-interval guidelines for gastric cancer should be suggested considering individual risk based on age, severity of atrophy, H. pylori status, and DNA methylation pattern.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4597805PMC
http://dx.doi.org/10.15430/JCP.2015.20.3.172DOI Listing

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