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IGF-II 启动子特异性甲基化及其在卵巢上皮性癌中的表达及其与疾病特征的关系。

IGF-II promoter specific methylation and expression in epithelial ovarian cancer and their associations with disease characteristics.

机构信息

Department of Epidemiology and Public Health, Yale Cancer Center, Yale University School of Medicine, New Haven, CT 06520-8034, USA.

出版信息

Oncol Rep. 2011 Jan;25(1):203-13.

Abstract

High expression of insulin-like growth factor-II (IGF-II) in epithelial ovarian cancer is associated with aggressive disease and poor prognosis. IGF-II transcription is initiated from multiple promoters. Promoter-specific expression is regulated by DNA methylation, which is often dysregulated in cancer. Here, the effects of promoter-specific methylation on IGF-II expression are investigated in ovarian cancer. Fresh tumor samples were collected from 211 patients for analyses of IGF-II promoter methylation using methylation-specific PCR, and of promoter-specific expression of IGF-II mRNA with qRT-PCR, as well as tissue levels of IGF-II peptide with an ELISA. Cox regression analysis was performed to assess IGF-II methylation and expression in association with progression-free and overall survival. DNA methylation was high in IGF-II promoters 2 (P2, 64.2%) and 3 (P3, 52.1%) and low in promoter 4 (P4, 9.8%). High methylation was associated with low mRNA expression in a promoter-specific manner. P3 methylation and expression appeared to be critical in ovarian cancer compared to other promoters. While methylation in an individual promoter was not associated with the disease, a methylation pattern involving P2 and P3 was significantly different among patients with distinct tumor grade, debulking results, residual tumor size and treatment response. The methylation pattern was also associated with disease progression. The study suggests that DNA methylation regulates IGF-II promoter-specific expression in ovarian cancer and the regulation may play a role in disease progression. Assessing methylation patterns in IGF-II promoters may have clinical implications.

摘要

胰岛素样生长因子-II(IGF-II)在卵巢上皮性癌中的高表达与侵袭性疾病和不良预后相关。IGF-II 的转录起始于多个启动子。启动子特异性表达受 DNA 甲基化调控,而 DNA 甲基化在癌症中常失调。本研究旨在探讨 IGF-II 表达的启动子特异性甲基化在卵巢癌中的作用。收集了 211 例新鲜肿瘤样本,采用甲基化特异性 PCR 分析 IGF-II 启动子甲基化,qRT-PCR 分析 IGF-II mRNA 的启动子特异性表达,ELISA 分析 IGF-II 肽的组织水平。采用 Cox 回归分析评估 IGF-II 甲基化和表达与无进展生存期和总生存期的关系。IGF-II 启动子 2(P2,64.2%)和 3(P3,52.1%)的 DNA 甲基化水平较高,而启动子 4(P4,9.8%)的甲基化水平较低。高甲基化与启动子特异性低 mRNA 表达相关。与其他启动子相比,P3 甲基化和表达似乎在卵巢癌中更为关键。虽然单个启动子的甲基化与疾病无关,但具有 P2 和 P3 甲基化特征的模式在不同肿瘤分级、减瘤结果、残留肿瘤大小和治疗反应的患者中存在显著差异。该甲基化模式与疾病进展相关。研究表明,DNA 甲基化调控卵巢癌中 IGF-II 启动子特异性表达,这种调控可能在疾病进展中发挥作用。评估 IGF-II 启动子的甲基化模式可能具有临床意义。

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