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结直肠癌(晚期)腺瘤中与癌症相关的 DNA 拷贝数事件的评估。

Evaluation of Cancer-Associated DNA Copy Number Events in Colorectal (Advanced) Adenomas.

机构信息

Department of Pathology, Netherlands Cancer Institute, Amsterdam, the Netherlands.

Department of Gastroenterology, Jeroen Bosch Hospital, 's-Hertogenbosch, the Netherlands.

出版信息

Cancer Prev Res (Phila). 2018 Jul;11(7):403-412. doi: 10.1158/1940-6207.CAPR-17-0317. Epub 2018 Apr 23.

Abstract

About 5% of colorectal adenomas are estimated to progress to colorectal cancer. However, it is important to identify which adenomas actually carry a high risk of progression, because these serve as intermediate endpoints, for example, in screening programs. In clinical practice, adenomas with a size of ≥10 mm, villous component and/or high-grade dysplasia, called advanced adenomas, are considered high risk, although solid evidence for this classification is lacking. Specific DNA copy number changes are associated with adenoma-to-carcinoma progression. We set out to determine the prevalence of cancer-associated events (CAE) in advanced and nonadvanced adenomas. DNA copy number analysis was performed on archival tissues from three independent series of, in total, 297 adenomas (120 nonadvanced and 177 advanced) using multiplex ligation-dependent probe amplification or low-coverage whole-genome DNA sequencing. Alterations in two or more CAEs were considered to mark adenomas as high risk. Two or more CAEs were overall present in 25% (95% CI, 19.0-31.8) of advanced adenomas; 23% (11/48), 36% (12/33), and 23% (22/96) of the advanced adenomas in series 1, 2, and 3, respectively, and 1.7% (1/58) and 4.8% (3/62) of the nonadvanced adenomas, in series 1 and 2, respectively. The majority of advanced adenomas do not show CAEs, indicating that only a subset of these lesions is to be considered high risk. Nonadvanced adenomas have very low prevalence of CAEs, although those with CAEs should be considered high risk as well. Specific DNA copy number alterations may better reflect the true progression risk than the advanced adenoma phenotype. .

摘要

约 5%的结直肠腺瘤估计会进展为结直肠癌。然而,重要的是要确定哪些腺瘤实际上具有进展为高危的风险,因为这些腺瘤作为中间终点,例如在筛查计划中。在临床实践中,直径≥10mm、绒毛成分和/或高级别异型增生的腺瘤被认为是高危腺瘤,称为高级别腺瘤,尽管缺乏这种分类的具体证据。特定的 DNA 拷贝数改变与腺瘤向癌的进展相关。我们旨在确定高级别和非高级别腺瘤中癌症相关事件 (CAE) 的发生率。使用多重连接依赖性探针扩增或低覆盖度全基因组 DNA 测序,对三个独立系列共 297 个腺瘤(120 个非高级别和 177 个高级别)的存档组织进行了 DNA 拷贝数分析。两个或多个 CAE 的改变被认为标志着腺瘤具有高风险。高级别腺瘤中总体存在两个或更多 CAE 的比例为 25%(95%CI,19.0-31.8);三个系列中的高级别腺瘤分别为 23%(11/48)、36%(12/33)和 23%(22/96),而在两个系列中分别有 1.7%(1/58)和 4.8%(3/62)的非高级别腺瘤存在两个或更多 CAE。大多数高级别腺瘤没有 CAE,这表明这些病变只有一部分被认为是高风险的。非高级别腺瘤 CAE 的发生率非常低,但也应将其视为高风险。特定的 DNA 拷贝数改变可能比高级别腺瘤表型更能反映真实的进展风险。

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