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使用纳米孔测序对患者基因组中的结构变异进行图谱绘制和相位分析。

Mapping and phasing of structural variation in patient genomes using nanopore sequencing.

机构信息

Department of Genetics, Center for Molecular Medicine, University Medical Center Utrecht, Utrecht University, 3584 CG, Utrecht, The Netherlands.

Medical Genetics Unit, Department of Clinical and Biological Sciences, University of Torino, Orbassano, 10043, Italy.

出版信息

Nat Commun. 2017 Nov 6;8(1):1326. doi: 10.1038/s41467-017-01343-4.

Abstract

Despite improvements in genomics technology, the detection of structural variants (SVs) from short-read sequencing still poses challenges, particularly for complex variation. Here we analyse the genomes of two patients with congenital abnormalities using the MinION nanopore sequencer and a novel computational pipeline-NanoSV. We demonstrate that nanopore long reads are superior to short reads with regard to detection of de novo chromothripsis rearrangements. The long reads also enable efficient phasing of genetic variations, which we leveraged to determine the parental origin of all de novo chromothripsis breakpoints and to resolve the structure of these complex rearrangements. Additionally, genome-wide surveillance of inherited SVs reveals novel variants, missed in short-read data sets, a large proportion of which are retrotransposon insertions. We provide a first exploration of patient genome sequencing with a nanopore sequencer and demonstrate the value of long-read sequencing in mapping and phasing of SVs for both clinical and research applications.

摘要

尽管基因组学技术不断改进,但从短读测序中检测结构变体(SVs)仍然具有挑战性,特别是对于复杂的变异。在这里,我们使用 MinION 纳米孔测序仪和一种新的计算管道-NanoSV 来分析两个患有先天性异常的患者的基因组。我们证明,与短读相比,纳米孔长读在检测从头发生的染色体重排方面具有优势。长读还能够有效地进行遗传变异的相位分析,我们利用这一点来确定所有从头发生的染色体重排断点的亲本来源,并解析这些复杂重排的结构。此外,对遗传 SVs 的全基因组监测揭示了新的变异,这些变异在短读数据集被遗漏,其中很大一部分是逆转录转座子插入。我们首次探索了使用纳米孔测序仪对患者基因组进行测序,并证明了长读测序在临床和研究应用中对 SVs 的映射和相位分析的价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3384/5673902/d7172d82eb7e/41467_2017_1343_Fig1_HTML.jpg

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