High-resolution array comparative genomic hybridization in sporadic and celiac disease-related small bowel adenocarcinomas

Begoña Diosdado; Tineke E Buffart; Russell Watkins; Beatriz Carvalho; Bauke Ylstra; Marianne Tijssen; Anne S Bolijn; Fraser Lewis; Karen Maude; Caroline Verbeke; Iris D Nagtegaal; Heike Grabsch; Chris J J Mulder; Phil Quirke; Peter Howdle; Gerrit A Meijer

doi:10.1158/1078-0432.CCR-09-1773

High-resolution array comparative genomic hybridization in sporadic and celiac disease-related small bowel adenocarcinomas

Clin Cancer Res. 2010 Mar 1;16(5):1391-401. doi: 10.1158/1078-0432.CCR-09-1773. Epub 2010 Feb 23.

Authors

Begoña Diosdado¹, Tineke E Buffart, Russell Watkins, Beatriz Carvalho, Bauke Ylstra, Marianne Tijssen, Anne S Bolijn, Fraser Lewis, Karen Maude, Caroline Verbeke, Iris D Nagtegaal, Heike Grabsch, Chris J J Mulder, Phil Quirke, Peter Howdle, Gerrit A Meijer

Affiliation

¹ Departments of Pathology and Gastroenterology, VU University Medical Center, Amsterdam, The Netherlands. b.diosdado@vumc.nl

PMID: 20179237
DOI: 10.1158/1078-0432.CCR-09-1773

Abstract

Purpose: The molecular pathogenesis of small intestinal adenocarcinomas is not well understood. Understanding the molecular characteristics of small bowel adenocarcinoma may lead to more effective patient treatment.

Experimental design: Forty-eight small bowel adenocarcinomas (33 non-celiac disease related and 15 celiac disease related) were characterized for chromosomal aberrations by high-resolution array comparative hybridization, microsatellite instability, and APC promoter methylation and mutation status. Findings were compared with clinicopathologic and survival data. Furthermore, molecular alterations were compared between celiac disease-related and non-celiac disease-related small bowel adenocarcinomas.

Results: DNA copy number changes were observed in 77% small bowel adenocarcinomas. The most frequent DNA copy number changes found were gains on 5p15.33-5p12, 7p22.3-7q11.21, 7q21.2-7q21.3, 7q22.1-7q34, 7q36.1, 7q36.3, 8q11.21-8q24.3, 9q34.11-9q34.3, 13q11-13q34, 16p13.3, 16p11.2, 19q13.2, and 20p13-20q13.33, and losses on 4p13-4q35.2, 5q15-5q21.1, and 21p11.2-21q22.11. Seven highly amplified regions were identified on 6p21.1, 7q21.1, 8p23.1, 11p13, 16p11.2, 17q12-q21.1, and 19q13.2. Celiac disease-related and non-celiac disease-related small bowel adenocarcinomas displayed similar chromosomal aberrations. Promoter hypermethylation of the APC gene was found in 48% non-celiac disease-related and 73% celiac disease-related small bowel adenocarcinomas. No nonsense mutations were found. Thirty-three percent of non-celiac disease-related small bowel adenocarcinomas showed microsatellite instability, whereas 67% of celiac disease-related small bowel adenocarcinomas were microsatellite unstable.

Conclusions: Our study characterized chromosomal aberrations and amplifications involved in small bowel adenocarcinoma. At the chromosomal level, celiac disease-related and non-celiac disease-related small bowel adenocarcinomas did not differ. A defect in the mismatch repair pathways seems to be more common in celiac disease-related than in non-celiac disease-related small bowel adenocarcinomas. In contrast to colon and gastric cancers, no APC nonsense mutations were found in small bowel adenocarcinoma. However, APC promoter methylation seems to be a common event in celiac disease-related small bowel adenocarcinoma. Clin Cancer Res; 16(5); 1391-401.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenocarcinoma / genetics*
Adenocarcinoma / mortality
Adult
Aged
Aged, 80 and over
Celiac Disease / complications*
Celiac Disease / genetics
Comparative Genomic Hybridization
DNA Methylation
Female
Gene Dosage
Genes, APC
Humans
Immunohistochemistry
Intestinal Neoplasms / genetics*
Intestinal Neoplasms / mortality
Kaplan-Meier Estimate
Male
Microsatellite Instability
Middle Aged
Promoter Regions, Genetic