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肺癌中的DNA甲基化模式。

DNA methylation patterns in lung carcinomas.

作者信息

Pfeifer Gerd P, Rauch Tibor A

机构信息

Department of Biology, Beckman Research Institute of the City of Hope, 1500 East Duarte Road, Duarte, CA 91010, USA.

出版信息

Semin Cancer Biol. 2009 Jun;19(3):181-7. doi: 10.1016/j.semcancer.2009.02.008. Epub 2009 Feb 20.

Abstract

The genome of epithelial tumors is characterized by numerous chromosomal aberrations, DNA base sequence changes, and epigenetic abnormalities. The epigenome of cancer cells has been most commonly studied at the level of DNA CpG methylation. In squamous cell carcinomas of the lung, CpG methylation patterns undergo substantial changes relative to normal lung epithelium. Using a genome-scale mapping technique for CpG methylation (MIRA-chip), we characterized CpG island methylation and methylation patterns of entire chromosome arms at a level of resolution of approximately 100 bp. In individual stage I lung carcinomas, several hundred and probably up to a thousand CpG islands become methylated. Interestingly, a large fraction (almost 80%) of the tumor-specifically methylated sequences are targets of the Polycomb complex in embryonic stem cells. Homeobox genes are particularly overrepresented and all four HOX gene loci on chromosomes 2, 7, 12, and 17 are hotspots for tumor-associated methylation because of the presence of multiple methylated CpG islands within these loci. DNA hypomethylation at CpGs in squamous cell tumors preferentially affects repetitive sequence classes including SINEs, LINEs, subtelomeric repeats, and segmental duplications. Since these epigenetic changes are found in early stage tumors, their contribution to tumor etiology as well as their potential usefulness as diagnostic or prognostic biomarkers of the disease should be considered.

摘要

上皮性肿瘤的基因组具有众多染色体畸变、DNA碱基序列变化和表观遗传异常的特征。癌细胞的表观基因组最常从DNA CpG甲基化水平进行研究。在肺鳞状细胞癌中,相对于正常肺上皮,CpG甲基化模式发生了显著变化。我们使用一种用于CpG甲基化的基因组规模映射技术(MIRA芯片),在大约100 bp的分辨率水平上对CpG岛甲基化和整条染色体臂的甲基化模式进行了表征。在单个I期肺癌中,数百个甚至可能多达一千个CpG岛发生甲基化。有趣的是,很大一部分(几乎80%)肿瘤特异性甲基化序列是胚胎干细胞中多梳蛋白复合体的靶标。同源框基因尤其富集,并且由于2号、7号、12号和17号染色体上的所有四个HOX基因座内存在多个甲基化的CpG岛,这些基因座是肿瘤相关甲基化的热点。鳞状细胞肿瘤中CpG处的DNA低甲基化优先影响包括短散在核元件、长散在核元件、亚端粒重复序列和节段重复序列在内的重复序列类别。由于这些表观遗传变化在早期肿瘤中就已发现,因此应考虑它们对肿瘤病因的贡献以及它们作为该疾病诊断或预后生物标志物的潜在用途。

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