Barrett's Esophagus

Morales, Thomas G.; Sampliner, Richard E.

doi:10.1001/archinte.159.13.1411

Cited by 47 publications

(1 citation statement)

References 37 publications

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“…Barrett’s esophagus is therefore of considerable clinical significance since the five-year survival rate of esophageal adenocarcinoma is only ~10%, unless detected at an early stage, in which case it is curable. It is therefore recommended that BE patients be managed by endoscopic surveillance; however, at present 95% of patients with esophageal adenocarcinoma do not have a prior diagnosis of Barrett’s esophagus (4). It is therefore important to define biomarkers which could be readily applied to patients with GERD to identify those who have BE and are at risk for EA, and would therefore benefit from endoscopic surveillance and/or medical or surgical intervention.…”

Section: Introductionmentioning

confidence: 99%

Deletion at Fragile Sites Is a Common and Early Event in Barrett's Esophagus

Lai

Kostadinov

Barrett

et al. 2010

Molecular Cancer Research

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Barrett’s esophagus is a premalignant intermediate to esophageal adenocarcinoma, which develops in the context of chronic inflammation and exposure to bile and acid. We asked whether there might be common genomic alterations that could be identified as potential clinical biomarker(s) for Barrett’s esophagus by whole genome profiling. We detected copy number alterations and/or loss of heterozygosity (LOH) at fifty-six fragile sites in 20 patients with premalignant Barrett’s esophagus (BE). Chromosomal fragile sites are particularly sensitive to DNA breaks and have been shown to be frequent sites of rearrangement or loss in many human cancers. 78% of all genomic alterations detected by array-CGH were associated with fragile sites. Copy number losses in early BE were observed at particularly high frequency at FRA3B (81%), FRA9A/C (71.4%), FRA5E (52.4%) and FRA 4D (52.4%), and at lower frequencies in other fragile sites, including FRA1K (42.9%), FRAXC (42.9%), FRA 12B (33.3%) and FRA16D (33.3%). Due to the consistency of the region of copy number loss, we were able to verify these results by quantitative PCR which detected loss of FRA3B and FRA16D, in 83% and 40% of early molecular stage BE patients respectively. LOH in these cases was confirmed via pyrosequencing at FRA3B and FRA16D (75% and 70% respectively). Deletion and genomic instability at FRA3B and other fragile sites could thus be a biomarker of genetic damage in BE patients and a potential biomarker of cancer risk.

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Section: Introductionmentioning

confidence: 99%