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Linkage disequilibrium maps to guide contig ordering for genome assembly

机译:连接不平衡贴图以引导基因组组件的折叠排序

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Motivation: Efforts to establish reference genome sequences by de novo sequence assembly have to address the difficulty of linking relatively short sequence contigs to form much larger chromosome assemblies. Efficient strategies are required to span gaps and establish contig order and relative orientation. We consider here the use of linkage disequilibrium (LD) maps of sequenced contigs and the utility of LD for ordering, orienting and positioning linked sequences. LD maps are readily constructed from population data and have at least an order of magnitude higher resolution than linkage maps providing the potential to resolve difficult areas in assemblies. We empirically evaluate a linkage disequilibrium map-based method using single nucleotide polymorphism genotype data in a 216 kilobase region of human 6p21.3 from which three shorter contigs are formed.
机译:动机:通过Novo序列组件建立参考基因组序列的努力必须解决连接相对短的序列Contig的难以形成更大的染色体组件。 需要高效的策略来跨越差距并建立Contig命令和相对方向。 我们考虑以下使用测序的Contigs的联动不平衡(LD)映射和LD的效用用于订购,定向和定位链接序列。 LD映射容易从人口数据构建,并且具有比连锁图更高的分辨率,提供潜力来解决组件中的困难区域。 我们在人6p21.3的216千碱基区域中使用单核苷酸多态性基因型数据凭经上评估了基于连锁的基于型映射的方法,从中形成了三个较短的折叠。

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