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BAsE-Seq: a method for obtaining long viral haplotypes from short sequence reads

机译:BAsE-Seq:一种从短序列读取中获得长病毒单倍型的方法

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摘要

We present a method for obtaining long haplotypes, of over 3 kb in length, using a short-read sequencer, Barcode-directed Assembly for Extra-long Sequences (BAsE-Seq). BAsE-Seq relies on transposing a template-specific barcode onto random segments of the template molecule and assembling the barcoded short reads into complete haplotypes. We applied BAsE-Seq on mixed clones of hepatitis B virus and accurately identified haplotypes occurring at frequencies greater than or equal to 0.4%, with >99.9% specificity. Applying BAsE-Seq to a clinical sample, we obtained over 9,000 viral haplotypes, which provided an unprecedented view of hepatitis B virus population structure during chronic infection. BAsE-Seq is readily applicable for monitoring quasispecies evolution in viral diseases.
机译:我们提出了一种使用短读音序器,超长序列的条形码指导程序集(BAsE-Seq)获得长单倍型,长度超过3 kb的方法。 BAsE-Seq依赖于将模板特异性条形码转码到模板分子的随机片段上,并将条形码短读组装成完整的单倍型。我们将BAsE-Seq应用到乙型肝炎病毒的混合克隆中,并准确鉴定了以大于或等于0.4%的频率出现的单倍型,其特异性> 99.9%。将BAsE-Seq应用于临床样本,我们获得了9,000多种病毒单倍型,这为慢性感染期间的乙型肝炎病毒种群结构提供了前所未有的视角。 BAsE-Seq可轻松应用于监测病毒性疾病的准物种进化。

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