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Probabilistic method for detecting copy number variation in a fetal genome using maternal plasma sequencing

机译:使用母体血浆测序检测胎儿基因组中拷贝数变异的概率方法

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Motivation: The past several years have seen the development of methodologies to identify genomic variation within a fetus through the non-invasive sequencing of maternal blood plasma. These methods are based on the observation that maternal plasma contains a fraction of DNA (typically 5-15%) originating from the fetus, and such methodologies have already been used for the detection of whole-chromosom events (aneuploidies), and to a more limited extent for smaller (typically several megabases long) copy number variants (CNVs). Results: Here we present a probabilistic method for non-invasive analysis of de novo CNVs in fetal genome based on maternal plasma sequencing. Our novel method combines three types of information within a unified Hidden Markov Model: the imbalance of allelic ratios at SNP positions, the use of parental genotypes to phase nearby SNPs and depth of coverage to better differentiate between various types of CNVs and improve precision. Our simulation results, based on in silico introduction of novel CNVs into plasma samples with 13% fetal DNA concentration, demonstrate a sensitivity of 90% for CNVs 4400 kb (with 13 calls in an unaffected genome), and 40% for 50- 400 kb CNVs (with 108 calls in an unaffected genome).
机译:动机:过去几年中,通过母体血浆的非侵入性测序鉴定胎儿基因组变异的方法学不断发展。这些方法是基于以下观察结果:母体血浆中含有一部分来自胎儿的DNA(通常为5-15%),这种方法已经用于检测全染色体事件(非整倍性),甚至更多。较小(通常长几个兆碱基)的拷贝数变体(CNV)的范围有限。结果:在这里,我们提出了一种基于母体血浆测序的无创分析胎儿基因组中新生CNV的概率方法。我们的新方法在统一的隐马尔可夫模型中结合了三种类型的信息:SNP位置等位基因比率的不平衡,使用亲本基因型对附近的SNP进行相移以及覆盖深度,以更好地区分各种CNV,并提高精度。我们的模拟结果基于在胎儿DNA浓度为13%的血浆样本中计算机模拟导入新型CNV的结果,表明对4400 kb的CNV(未受影响的基因组有13个调用)的敏感性为90%,对50- 400 kb的CNV的敏感性为40% CNV(在不受影响的基因组中有108个调用)。

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