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Extensive and deep sequencing of the Venter/HuRef genome for developing and benchmarking genome analysis tools

机译:Venter / HuRef基因组的广泛和深度测序用于开发和对标基因组分析工具

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摘要

We produced an extensive collection of deep re-sequencing datasets for the Venter/HuRef genome using the Illumina massively-parallel DNA sequencing platform. The original Venter genome sequence is a very-high quality phased assembly based on Sanger sequencing. Therefore, researchers developing novel computational tools for the analysis of human genome sequence variation for the dominant Illumina sequencing technology can test and hone their algorithms by making variant calls from these Venter/HuRef datasets and then immediately confirm the detected variants in the Sanger assembly, freeing them of the need for further experimental validation. This process also applies to implementing and benchmarking existing genome analysis pipelines. We prepared and sequenced 200 bp and 350 bp short-insert whole-genome sequencing libraries (sequenced to 100x and 40x genomic coverages respectively) as well as 2 kb, 5 kb, and 12 kb mate-pair libraries (49x, 122x, and 145x physical coverages respectively). Lastly, we produced a linked-read library (128x physical coverage) from which we also performed haplotype phasing.
机译:我们使用Illumina大规模平行DNA测序平台为Venter / HuRef基因组产生了广泛的深度重测序数据集。最初的Venter基因组序列是基于Sanger测序的非常高质量的分阶段装配。因此,研究人员开发了新颖的计算工具来分析占主导地位的Illumina测序技术的人类基因组序列变异,可以通过从这些Venter / HuRef数据集中进行变异调用来测试并磨练其算法,然后立即在Sanger装配中确认检测到的变异,从而释放出他们需要进一步的实验验证。此过程还适用于实施和对现有基因组分析管道进行基准测试。我们准备并测序了200 bp和350 bp的短插入全基因组测序文库(分别测序为100x和40x基因组覆盖率)以及2 kb,5 kb和12 kb伴侣对文库(49x,122x和145x)物理覆盖范围)。最后,我们生成了一个链接阅读的库(物理覆盖率是128倍),从中我们还执行了单倍型定相。

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