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CoLoRMap: Correcting Long Reads by Mapping short reads

机译:CoLoRMap:通过映射短读来纠正长读

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Motivation: Second generation sequencing technologies paved the way to an exceptional increase in the number of sequenced genomes, both prokaryotic and eukaryotic. However, short reads are difficult to assemble and often lead to highly fragmented assemblies. The recent developments in long reads sequencing methods offer a promising way to address this issue. However, so far long reads are characterized by a high error rate, and assembling from long reads require a high depth of coverage. This motivates the development of hybrid approaches that leverage the high quality of short reads to correct errors in long reads.
机译:动机:第二代测序技术为原核和真核测序基因组数目的异常增加铺平了道路。然而,短读段难以组装,并且经常导致高度零散的组装。长读测序方法的最新发展为解决此问题提供了一种有希望的方法。然而,到目前为止,长读取的特征在于高错误率,并且从长读取进行组装需要较高的覆盖深度。这激励了混合方法的发展,该方法利用短读的高质量来纠正长读中的错误。

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