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Comparison of cancer-associated genetic abnormalities in columnar-lined esophagus tissues with and without goblet cells. | LitMetric

Comparison of cancer-associated genetic abnormalities in columnar-lined esophagus tissues with and without goblet cells.

Ann Surg

*Departments of Surgery ‡Pathology, and ‖Biostatistics, University of Rochester Medical Center, Strong Memorial Hospital, Rochester, NY †Life Technologies, Foster City, CA **Dana Farber Cancer Center, Boston, MA ††University of Michigan, Ann Arbor, MI ¶University of Pittsburgh, Pittsburgh, PA; and §Department of Surgery, Boston University, Boston, MA.

Published: July 2014

AI Article Synopsis

  • The study aimed to compare the genetic abnormalities present in esophageal metaplasia biopsies with goblet cells (intestinal metaplasia or IM) and those without (nongoblet cell metaplasia or NGM) to evaluate their association with esophageal adenocarcinoma (EAC) risk.
  • Researchers analyzed DNA from 90 biopsies and found significant copy number abnormalities linked to cancer in IM samples, while NGM showed no such changes.
  • The findings indicate that IM has a much higher frequency of cancer-related genetic mutations compared to NGM, suggesting that these metaplastic types may carry different risks for developing EAC.

Article Abstract

Objective: To determine and compare the frequency of cancer-associated genetic abnormalities in esophageal metaplasia biopsies with and without goblet cells.

Background: Barrett's esophagus is associated with increased risk of esophageal adenocarcinoma (EAC), but the appropriate histologic definition of Barrett's esophagus is debated. Intestinal metaplasia (IM) is defined by the presence of goblet cells whereas nongoblet cell metaplasia (NGM) lacks goblet cells. Both have been implicated in EAC risk but this is controversial. Although IM is known to harbor genetic changes associated with EAC, little is known about NGM. We hypothesized that if NGM and IM infer similar EAC risk, then they would harbor similar genetic aberrations in genes associated with EAC.

Methods: Ninety frozen NGM, IM, and normal tissues from 45 subjects were studied. DNA copy number abnormalities were identified using microarrays and fluorescence in situ hybridization. Targeted sequencing of all exons from 20 EAC-associated genes was performed on metaplasia biopsies using Ion AmpliSeq DNA sequencing.

Results: Frequent copy number abnormalities targeting cancer-associated genes were found in IM whereas no such changes were observed in NGM. In 1 subject, fluorescence in situ hybridization confirmed loss of CDKN2A and amplification of chromosome 8 in IM but not in a nearby NGM biopsy. Targeted sequencing revealed 11 nonsynonymous mutations in 16 IM samples and 2 mutations in 19 NGM samples.

Conclusions: This study reports the largest and most comprehensive comparison of DNA aberrations in IM and NGM genomes. Our results show that IM has a much higher frequency of cancer-associated mutations than NGM.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4047149PMC
http://dx.doi.org/10.1097/SLA.0000000000000424DOI Listing

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