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Accurate and reliable high-throughput detection of copy number variation in the human genome

机译:准确可靠的高通量检测人类基因组拷贝数变异

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摘要

This study describes a new tool for accurate and reliable high-throughput detection of copy number variation in the human genome. We have constructed a large-insert clone DNA microarray covering the entire human genome in tiling path resolution that we have used to identify copy number variation in human populations. Crucial to this study has been the development of a robust array platform and analytic process for the automated identification of copy number variants (CNVs). The array consists of 26,574 clones covering 93.7% of euchromatic regions. Clones were selected primarily from the published “Golden Path,” and mapping was confirmed by fingerprinting and BAC-end sequencing. Array performance was extensively tested by a series of validation assays. These included determining the hybridization characteristics of each individual clone on the array by chromosome-specific add-in experiments. Estimation of data reproducibility and false-positiveegative rates was carried out using self–self hybridizations, replicate experiments, and independent validations of CNVs. Based on these studies, we developed a variance-based automatic copy number detection analysis process (CNVfinder) and have demonstrated its robustness by comparison with the SW-ARRAY method.
机译:这项研究描述了一种新工具,用于准确,可靠地高通量检测人类基因组中的拷贝数变异。我们构建了一个大插入克隆DNA微阵列,该阵列以平铺路径分辨率覆盖了整个人类基因组,我们已经使用该阵列来识别人类种群中的拷贝数变异。这项研究的关键是开发一个强大的阵列平台和用于自动识别拷贝数变异(CNV)的分析过程。该阵列由26,574个克隆组成,覆盖了93.7%的常染色体区域。主要从公开的“黄金路径”中选择克隆,并通过指纹图谱和BAC末端测序确认映射。阵列性能已通过一系列验证测定法进行了广泛测试。这些措施包括通过染色体特异性附加实验确定阵列上每个单独克隆的杂交特征。数据重现性和假阳性/阴性率的估计是使用自我-自我杂交,重复实验和CNV的独立验证进行的。基于这些研究,我们开发了基于差异的自动拷贝数检测分析过程(CNVfinder),并通过与SW-ARRAY方法进行比较证明了其鲁棒性。

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