散发性和乳糜泻相关小肠腺癌中高分辨率阵列比较基因组杂交。

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

机构信息

Departments of Pathology and Gastroenterology, VU University Medical Center, Amsterdam, The Netherlands.

出版信息

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

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

PMID:20179237

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.

摘要

目的

小肠腺癌的分子发病机制尚不清楚。了解小肠腺癌的分子特征可能会导致更有效的患者治疗。

实验设计

对 48 例小肠腺癌（33 例非麸质相关疾病和 15 例麸质相关疾病）进行高分辨率微阵列比较杂交、微卫星不稳定性和 APC 启动子甲基化和突变状态分析，以确定染色体畸变。将研究结果与临床病理和生存数据进行比较。此外，还比较了麸质相关疾病和非麸质相关疾病小肠腺癌之间的分子改变。

结果

在 77%的小肠腺癌中观察到 DNA 拷贝数变化。发现最常见的 DNA 拷贝数变化是 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 和 20p13-20q13.33 的增益，以及 4p13-4q35.2、5q15-5q21.1 和 21p11.2-21q22.11 的缺失。在 6p21.1、7q21.1、8p23.1、11p13、16p11.2、17q12-q21.1 和 19q13.2 上鉴定出 7 个高度扩增区域。非麸质相关疾病的小肠腺癌中发现 APC 基因启动子超甲基化 48%，而麸质相关疾病的小肠腺癌中发现 73%。未发现无义突变。非麸质相关疾病的小肠腺癌中有 33%表现出微卫星不稳定性，而麸质相关疾病的小肠腺癌中有 67%表现出微卫星不稳定性。

结论

本研究描述了小肠腺癌中涉及的染色体畸变和扩增。在染色体水平上，麸质相关疾病和非麸质相关疾病的小肠腺癌没有差异。错配修复途径的缺陷似乎在麸质相关疾病的小肠腺癌中比在非麸质相关疾病的小肠腺癌中更为常见。与结肠和胃癌不同，在小肠腺癌中未发现 APC 无义突变。然而，APC 启动子甲基化似乎是麸质相关疾病的小肠腺癌中的常见事件。临床癌症研究；16（5）；1391-401。