人胃癌相关的 9 个 miR CpG 岛甲基化特征及其在体外和体内对表达的抑制作用。
Characterization of human gastric carcinoma-related methylation of 9 miR CpG islands and repression of their expressions in vitro and in vivo.
机构信息
Key Laboratory of Carcinogenesis and Translational Research, Ministry of Education, Division of Cancer Etiology, Peking University Cancer Hospital and Institute, Fu-Cheng-Lu, No,52 Haidian District, Beijing 100142, China.
出版信息
BMC Cancer. 2012 Jun 15;12:249. doi: 10.1186/1471-2407-12-249.
BACKGROUND
Many miR genes are located within or around CpG islands. It is unclear whether methylation of these CpG islands represses miR transcription regularly. The aims of this study are to characterize gastric carcinoma (GC)-related methylation of miR CpG islands and its relationship with miRNA expression.
METHODS
Methylation status of 9 representative miR CpG islands in a panel of cell lines and human gastric samples (including 13 normal biopsies, 38 gastritis biopsies, 112 pairs of GCs and their surgical margin samples) was analyzed by bisulfite-DHPLC and sequencing. Mature miRNA levels were determined with quantitative RT-PCR. Relationships between miR methylation, transcription, GC development, and clinicopathological characteristics were statistically analyzed.
RESULTS
Methylation frequency of 5 miR CpG islands (miR-9-1, miR-9-3, miR-137, miR-34b, and miR-210) gradually increased while the proportion of methylated miR-200b gradually decreased during gastric carcinogenesis (Ps < 0.01). More miR-9-1 methylation was detected in 62%-64% of the GC samples and 4% of the normal or gastritis samples (18/28 versus 2/48; Odds ratio, 41.4; P < 0.01). miR-210 methylation showed high correlation with H. pylori infection. miR-375, miR-203, and miR-193b methylation might be host adaptation to the development of GCs. Methylation of these miR CpG islands was consistently shown to significantly decrease the corresponding miRNA levels presented in human cell lines. The inverse relationship was also observed for miR-9-1, miR-9-3, miR-137, and miR-200b in gastric samples. Among 112 GC patients, miR-9-1 methylation was an independent favourable predictor of overall survival of GC patients in both univariate and multivariate analysis (P < 0.02).
CONCLUSIONS
In conclusion, alteration of methylation status of 6 of 9 tested miR CpG islands was characterized in gastric carcinogenesis. miR-210 methylation correlated with H. pylori infection. miR-9-1 methylation may be a GC-specific event. Methylation of miR CpG islands may significantly down-regulate their transcription regularly.
背景
许多 miR 基因位于 CpG 岛内部或周围。目前尚不清楚这些 CpG 岛的甲基化是否会常规抑制 miR 转录。本研究旨在分析胃癌(GC)相关 miR CpG 岛的甲基化及其与 miRNA 表达的关系。
方法
采用亚硫酸氢盐-DHPLC 和测序分析了一组细胞系和人胃样本(包括 13 个正常活检、38 个胃炎活检、112 对 GC 及其手术切缘样本)中 9 个代表性 miR CpG 岛的甲基化状态。采用定量 RT-PCR 测定成熟 miRNA 水平。统计学分析 miR 甲基化、转录、GC 发生与临床病理特征之间的关系。
结果
在胃癌发生过程中,5 个 miR CpG 岛(miR-9-1、miR-9-3、miR-137、miR-34b 和 miR-210)的甲基化频率逐渐升高,而 miR-200b 的甲基化比例逐渐降低(P<0.01)。在 62%-64%的 GC 样本中检测到 miR-9-1 甲基化,而在 4%的正常或胃炎样本中未检测到(18/28 与 2/48;比值比,41.4;P<0.01)。miR-210 甲基化与 H. pylori 感染高度相关。miR-375、miR-203 和 miR-193b 甲基化可能是宿主对 GC 发生的适应。这些 miR CpG 岛的甲基化与相应 miRNA 水平在人细胞系中的显著降低有关。在胃样本中也观察到 miR-9-1、miR-9-3、miR-137 和 miR-200b 的负相关关系。在 112 例 GC 患者中,miR-9-1 甲基化在单因素和多因素分析中均是 GC 患者总生存的独立有利预测因子(P<0.02)。
结论
总之,在胃癌发生过程中,6 个检测到的 miR CpG 岛的甲基化状态发生了改变。miR-210 甲基化与 H. pylori 感染相关。miR-9-1 甲基化可能是 GC 特有的事件。miR CpG 岛的甲基化可能会常规下调其转录。
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