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REXTAL: Regional Extension of Assemblies Using Linked-Reads

机译:Rextal:使用链接阅读的集会区域延伸

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It is currently impossible to get complete de novo assembly of segmentally duplicated genome regions using genome-wide short-read datasets. Here, we devise a new computational method called Regional Extension of Assemblies Using Linked-Reads (REXTAL) for improved region-specific assembly of segmental duplication-containing DNA, leveraging genomic short-read datasets generated from large DNA molecules partitioned and barcoded using the Gel Bead in Emulsion (GEM) microfluidic method [1]. We show that using REXTAL, it is possible to extend assembly of single-copy diploid DNA into adjacent, otherwise inaccessible subtelomere segmental duplication regions and other subtelomeric gap regions. Moreover, REXTAL is computationally more efficient for the directed assembly of such regions from multiple genomes (e.g., for the comparison of structural variation) than genomewide assembly approaches.
机译:目前不可能使用基因组的短读数据集来完成分段重复的基因组区域的完整DE Novo组装。在这里,我们使用链接读取(Rextal)设计一种称为组件的区域扩展的新计算方法,用于改进含有分段复制的DNA的特定区域特征,利用从凝胶分配的大DNA分子产生的基因组短读数数据集乳液(宝石)微流体方法[1]。我们表明,使用Rextal,可以将单拷贝二倍体DNA的组装扩展到相邻,否则无法访问的子提示部分分段重复区域和其他子制度间隙区域。此外,Rextal用于从多个基因组的定向组装(例如,用于比较结构变化的比较)来计算地更有效地比基因组组装方法更高。

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