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首页> 外文期刊>BMC Bioinformatics >Linkage disequilibrium based genotype calling from low-coverage shotgun sequencing reads
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Linkage disequilibrium based genotype calling from low-coverage shotgun sequencing reads

机译:低覆盖散弹枪测序读取基于连锁不平衡的基因型

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Background Recent technology advances have enabled sequencing of individual genomes, promising to revolutionize biomedical research. However, deep sequencing remains more expensive than microarrays for performing whole-genome SNP genotyping. Results In this paper we introduce a new multi-locus statistical model and computationally efficient genotype calling algorithms that integrate shotgun sequencing data with linkage disequilibrium (LD) information extracted from reference population panels such as Hapmap or the 1000 genomes project. Experiments on publicly available 454, Illumina, and ABI SOLiD sequencing datasets suggest that integration of LD information results in genotype calling accuracy comparable to that of microarray platforms from sequencing data of low-coverage. A software package implementing our algorithm, released under the GNU General Public License, is available at http://dna.engr.uconn.edu/software/GeneSeq/. Conclusions Integration of LD information leads to significant improvements in genotype calling accuracy compared to prior LD-oblivious methods, rendering low-coverage sequencing as a viable alternative to microarrays for conducting large-scale genome-wide association studies.
机译:背景技术最近的技术进步已使单个基因组测序成为可能,有望彻底改变生物医学研究。然而,进行全基因组SNP基因分型的深度测序仍比微阵列昂贵。结果在本文中,我们介绍了一种新的多基因座统计模型和高效计算的基因型调用算法,该算法将shot弹枪测序数据与从参考群体(如Hapmap或1000个基因组计划)中提取的连锁不平衡(LD)信息相集成。对公开可用的454,Illumina和ABI SOLiD测序数据集进行的实验表明,LD信息的整合所产生的基因型检出准确度可与低覆盖率测序数据中的微阵列平台相媲美。可在http://dna.engr.uconn.edu/software/GeneSeq/处获得根据GNU通用公共许可发布的用于实现我们算法的软件包。结论LD信息的整合与以前的LD不了解的方法相比,可显着提高基因型调用的准确性,从而使低覆盖率测序成为微阵列进行大规模全基因组关联研究的可行选择。

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