在口腔和血液白细胞 DNA 中测量生物标记物,作为结肠组织全局甲基化的替代物。

International journal of molecular epidemiology and genetics Pub Date : 2014-05-29 eCollection Date: 2014-01-01
Janet E Ashbury, Sherryl A Taylor, M Yat Tse, Stephen C Pang, Jacob A Louw, Stephen J Vanner, Will D King
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引用次数: 0

摘要

越来越多的人希望弄清全球 DNA 甲基化水平在结直肠癌(CRC)病因学中的作用。在流行病学研究中,最常见的方法是测量血液白细胞中 DNA 的甲基化水平,以此作为结肠组织甲基化变化的替代指标。然而,人们对结肠组织 DNA 中的全局甲基化水平与血液或口腔细胞等更容易获得的组织之间的相关性知之甚少。这项横断面研究利用结肠镜筛查人群的 DNA 样本来确定非目标组织(如血液、口腔细胞)中的 LINE-1 甲基化水平(作为全基因组甲基化的代表)在多大程度上反映了直接面临患 CRC 风险的结肠粘膜组织的甲基化模式。在口腔和血液白细胞 DNA 中的 LINE-1 甲基化水平之间观察到最强的皮尔逊相关性(r = 0.50;N = 67),血液和结肠组织(r = 0.36;N = 280)以及口腔和结肠组织(r = 0.27;N = 72)之间的相关性较弱。这些弱/中等相关性的发现对于解释和规划未来的表观遗传标记物和 CRC 风险调查具有重要意义。
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Biomarkers measured in buccal and blood leukocyte DNA as proxies for colon tissue global methylation.

There is increasing interest in clarifying the role of global DNA methylation levels in colorectal cancer (CRC) etiology. Most commonly, in epidemiologic studies, methylation is measured in DNA derived from blood leukocytes as a proxy measure of methylation changes in colon tissue. However, little is known about the correlations between global methylation levels in DNA derived from colon tissue and more accessible tissues such as blood or buccal cells. This cross-sectional study utilized DNA samples from a screening colonoscopy population to determine to what extent LINE-1 methylation levels (as a proxy for genome-wide methylation) in non-target tissue (e.g., blood, buccal cells) reflected methylation patterns of colon mucosal tissue directly at risk of developing CRC. The strongest Pearson correlation was observed between LINE-1 methylation levels in buccal and blood leukocyte DNA (r = 0.50; N = 67), with weaker correlations for comparisons between blood and colon tissue (r = 0.36; N = 280), and buccal and colon tissue (r = 0.27; N = 72). These findings of weak/moderate correlations have important implications for interpreting and planning future investigations of epigenetic markers and CRC risk.

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