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Multi-genome Scaffold Co-assembly Based on the Analysis of Gene Orders and Genomic Repeats

机译:基于基因顺序和基因组重复分析的多基因组支架组装

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Advances in the DNA sequencing technology over the past decades have increased the volume of raw sequenced genomic data available for further assembly and analysis. While there exist many software tools for assembly of sequenced genomic material, they often experience difficulties with reconstructing complete chromosomes. Major obstacles include uneven read coverage and long similar subsequences (repeats) in genomes. Assemblers therefore often are able to reliably reconstruct only long subsequences, called scaffolds. We present a method for simultaneous co-assembly of all fragmented genomes (represented as collections of scaffolds rather than chromosomes) in a given set of annotated genomes. The method is based on the analysis of gene orders and relies on the evolutionary model, which includes genome rearrangements as well as gene insertions and deletions. It can also utilize information about genomic repeats and the phyloge-netic tree of the given genomes, further improving their assembly quality.
机译:在过去的几十年中,DNA测序技术的进步增加了可用于进一步组装和分析的原始测序基因组数据的数量。尽管存在许多用于组装测序的基因组材料的软件工具,但它们在重建完整染色体时经常遇到困难。主要障碍包括阅读覆盖率不均和基因组中较长的相似子序列(重复序列)。因此,组装人员通常只能可靠地重建仅称为支架的长子序列。我们提出了一种在给定的带注释基因组集中同时共同组装所有碎片基因组(表示为支架而不是染色体的集合)的方法。该方法基于对基因顺序的分析,并依赖于进化模型,该模型包括基因组重排以及基因的插入和缺失。它还可以利用有关给定基因组的基因组重复和系统进化树的信息,从而进一步提高其装配质量。

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