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CpG Island microarray probe sequences derived from a physical library are representative of CpG Islands annotated on the human genome

机译:源自物理文库的CpG Island微阵列探针序列代表在人类基因组上标注的CpG Islands

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摘要

An effective tool for the global analysis of both DNA methylation status and protein–chromatin interactions is a microarray constructed with sequences containing regulatory elements. One type of array suited for this purpose takes advantage of the strong association between CpG Islands (CGIs) and gene regulatory regions. We have obtained 20 736 clones from a CGI Library and used these to construct CGI arrays. The utility of this library requires proper annotation and assessment of the clones, including CpG content, genomic origin and proximity to neighboring genes. Alignment of clone sequences to the human genome (UCSC hg17) identified 9595 distinct genomic loci; 64% were defined by a single clone while the remaining 36% were represented by multiple, redundant clones. Approximately 68% of the loci were located near a transcription start site. The distribution of these loci covered all 23 chromosomes, with 63% overlapping a bioinformatically identified CGI. The high representation of genomic CGI in this rich collection of clones supports the utilization of microarrays produced with this library for the study of global epigenetic mechanisms and protein–chromatin interactions. A browsable database is available on-line to facilitate exploration of the CGIs in this library and their association with annotated genes or promoter elements.
机译:一种可对DNA甲基化状态和蛋白质-染色质相互作用进行全局分析的有效工具是构建了一个含有调控元件序列的微阵列。一种适合于此目的的阵列类型利用了CpG岛(CGI)与基因调控区之间的强关联。我们从CGI库中获得了20736个克隆,并用它们来构建CGI阵列。该库的实用程序要求对克隆进行适当的注释和评估,包括CpG含量,基因组起源和与邻近基因的接近度。克隆序列与人类基因组(UCSC hg17)的比对确定了9595个不同的基因组位点; 64%由单个克隆定义,其余36%由多个冗余克隆表示。大约68%的基因座位于转录起始位点附近。这些基因座的分布覆盖了所有23条染色体,其中63%与生物信息学鉴定的CGI重叠。在如此丰富的克隆集中,基因组CGI的高度代表性支持了利用该文库生产的微阵列来研究全球表观遗传机制和蛋白质-染色质相互作用。可在线浏览的数据库可促进对该库中CGI的探索及其与注释的基因或启动子元件的关联。

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