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PennCNV: An integrated hidden Markov model designed for high-resolution copy number variation detection in whole-genome SNP genotyping data

机译:PennCNV:一种集成的隐马尔可夫模型,设计用于全基因组SNP基因分型数据中的高分辨率拷贝数变异检测

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摘要

Comprehensive identification and cataloging of copy number variations (CNVs) is required to provide a complete view of human genetic variation. The resolution of CNV detection in previous experimental designs has been limited to tens or hundreds of kilobases. Here we present PennCNV, a hidden Markov model (HMM) based approach, for kilobase-resolution detection of CNVs from Illumina high-density SNP genotyping data. This algorithm incorporates multiple sources of information, including total signal intensity and allelic intensity ratio at each SNP marker, the distance between neighboring SNPs, the allele frequency of SNPs, and the pedigree information where available. We applied PennCNV to genotyping data generated for 112 HapMap individuals; on average, we detected ∼27 CNVs for each individual with a median size of ∼12 kb. Excluding common rearrangements in lymphoblastoid cell lines, the fraction of CNVs in offspring not detected in parents (CNV-NDPs) was 3.3%. Our results demonstrate the feasibility of whole-genome fine-mapping of CNVs via high-density SNP genotyping.
机译:需要对拷贝数变异(CNV)进行全面的识别和分类,以提供人类遗传变异的完整视图。在以前的实验设计中,CNV检测的分辨率仅限于几十或几百个千基。在这里,我们介绍PennCNV,这是一种基于隐马尔可夫模型(HMM)的方法,用于从Illumina高密度SNP基因分型数据中千碱基分辨率检测CNV。该算法结合了多种信息源,包括每个SNP标记处的总信号强度和等位基因强度比,相邻SNP之间的距离,SNP的等位基因频率以及可用的谱系信息。我们将PennCNV应用于为112个HapMap个体生成的基因分型数据。平均而言,我们为每个个体检测到约27个CNV,中位大小约为12 kb。除去淋巴母细胞样细胞系中常见的重排,在父母中未检测到的后代中CNV的比例为3.3%。我们的结果证明了通过高密度SNP基因分型对CNV进行全基因组精细映射的可行性。

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