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POPULATION SEQUENCING USING SHORT READS: HIV AS A CASE STUDY

机译:使用简短阅读人口测序:艾滋病毒是一个案例研究

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Despite many drawbacks, traditional sequencing technologies have proven to be invaluable in modern medical research, even when the targeted genomes are highly variable. While it is often known in such cases that multiple slightly different sequences are present in the analyzed sample in concentrations that vary dramatically, the traditional techniques typically allow only the most dominant strain to be extracted from a single chromatogram. These limitations made some research directions rather difficult to pursue. For example, the analysis of HIV evolution (including the emergence of drug resistance) in a single patient is expected to benefit from a comprehensive catalog of the patient's HIV population. In this paper, we show how the new generation of sequencing technologies, based on high throughput of short reads, can be used to link site variants and reconstruct multiple full strains of the targeted gene, including those of low concentration in the sample. Our algorithm is based on a generative model of the sequencing process, and uses a tailored probabilistic inference and learning procedure to fit the model to the obtained reads.
机译:尽管存在许多缺点,但即使当有针对性的基因组是高度变化的情况,传统的测序技术也已被证明是在现代医学研究中的宝贵。虽然在这种情况下通常已知在分析的样品中存在多个略微不同的序列,其浓度在急剧上变化,但传统的技术通常仅允许从单个色谱图中提取最大的菌株。这些限制使一些研究方向相当难以追求。例如,预计单个患者中HIV演化(包括耐药物的出现)的分析将受益于患者艾滋病毒群体的综合目录。在本文中,我们展示了基于高读数的高吞吐量的新一代测序技术如何用于链接位点变体并重建靶基因的多个全菌株,包括样品中低浓度的菌株。我们的算法基于测序过程的生成模型,并使用量身定制的概率推断和学习过程将模型拟合到所获得的读取。

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