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Array-based profiling of reference-independent methylation status (aPRIMES) identifies frequent promoter methylation and consecutive downregulation of ZIC2 in pediatric medulloblastoma

机译:基于阵列的参考无关甲基化状态(aPRIMES)谱分析确定了小儿髓母细胞瘤中频繁的启动子甲基化和ZIC2的连续下调

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摘要

Existing microarray-based approaches for screening of DNA methylation are hampered by a number of shortcomings, such as the introduction of bias by DNA copy-number imbalances in the test genome and negligence of tissue-specific methylation patterns. We developed a method designated array-based profiling of reference-independent methylation status (aPRIMES) that allows the detection of direct methylation status rather than relative methylation. Array-PRIMES is based on the differential restriction and competitive hybridization of methylated and unmethylated DNA by methylation-specific and methylation-sensitive restriction enzymes, respectively. We demonstrate the accuracy of aPRIMES in detecting the methylation status of CpG islands for different states of methylation. Application of aPRIMES to the DNA from desmoplastic medulloblastomas of monozygotic twins showed strikingly similar methylation profiles. Additional analysis of 18 sporadic medulloblastomas revealed an overall correlation between highly methylated tumors and poor clinical outcome and identified ZIC2 as a frequently methylated gene in pediatric medulloblastoma.
机译:现有的基于微阵列的DNA甲基化筛选方法受到许多缺点的阻碍,例如测试基因组中DNA拷贝数不平衡引起的偏倚和组织特异性甲基化模式的过失。我们开发了一种方法,该方法指定了与参考无关的甲基化状态(aPRIMES)的基于阵列的分析,该方法允许检测直接甲基化状态而不是相对甲基化。 Array-PRIMES分别基于甲基化特异性和甲基化敏感的限制性酶对甲基化和未甲基化DNA的差异限制和竞争性杂交。我们证明了aPRIMES在检测CpG岛甲基化状态对于不同甲基化状态方面的准确性。将aPRIMES应用于单卵双胞胎的增生性髓母细胞瘤的DNA表现出惊人的相似的甲基化特征。对18例散发性髓母细胞瘤的进一步分析显示,高度甲基化的肿瘤与不良的临床预后之间存在总体相关性,并确定ZIC2是小儿髓母细胞瘤中经常甲基化的基因。

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