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Methylation panel is a diagnostic biomarker for Barrett's oesophagus in endoscopic biopsies and non-endoscopic cytology specimens

Authors :
Hamza, Chettouh
Oliver, Mowforth
Núria, Galeano-Dalmau
Navya, Bezawada
Caryn, Ross-Innes
Shona, MacRae
Irene, Debiram-Beecham
Maria, O'Donovan
Rebecca C, Fitzgerald
Source :
Gut
Publication Year :
2017

Abstract

Objective Barrett’s oesophagus is a premalignant condition that occurs in the context of gastro-oesophageal reflux. However, most Barrett’s cases are undiagnosed because of reliance on endoscopy. We have developed a non-endoscopic tool: the Cytosponge, which when combined with trefoil factor 3 immunohistochemistry, can diagnose Barrett’s oesophagus. We investigated whether a quantitative methylation test that is not reliant on histopathological analysis could be used to diagnose Barrett’s oesophagus. Design Differentially methylated genes between Barrett’s and normal squamous oesophageal biopsies were identified from whole methylome data and confirmed using MethyLight PCR in biopsy samples of squamous oesophagus, gastric cardia and Barrett’s oesophagus. Selected genes were then tested on Cytosponge BEST2 trial samples comprising a pilot cohort (n=20 cases, n=10 controls) and a validation cohort (n=149 cases, n=129 controls). Results Eighteen genes were differentially methylated in patients with Barrett’soesophagus compared with squamous controls. Hypermethylation of TFPI2, TWIST1, ZNF345 and ZNF569 was confirmed in Barrett’s biopsies compared with biopsies from squamous oesophagus and gastric cardia (p

Details

ISSN :
14683288
Volume :
67
Issue :
11
Database :
OpenAIRE
Journal :
Gut
Accession number :
edsair.pmid..........fafa8dc5c0e03b9de018dca07cbe293b