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BM-map: Bayesian mapping of multireads for next-generation sequencing data.

by: Yuan Ji, Yanxun Xu, Qiong Zhang, Kam-Wah W. Tsui, Yuan Yuan, Clift Norris, Shoudan Liang, Han Liang
Biometrics, Vol. 67, No. 4. (22 December 2011), pp. 1215-1224, doi:10.1111/j.1541-0420.2011.01605.x  Key: citeulike:9219275

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Abstract

Next-generation sequencing (NGS) technology generates millions of short reads, which provide valuable information for various aspects of cellular activities and biological functions. A key step in NGS applications (e.g., RNA-Seq) is to map short reads to correct genomic locations within the source genome. While most reads are mapped to a unique location, a significant proportion of reads align to multiple genomic locations with equal or similar numbers of mismatches; these are called multireads. The ambiguity in mapping the multireads may lead to bias in downstream analyses. Currently, most practitioners discard the multireads in their analysis, resulting in a loss of valuable information, especially for the genes with similar sequences. To refine the read mapping, we develop a Bayesian model that computes the posterior probability of mapping a multiread to each competing location. The probabilities are used for downstream analyses, such as the quantification of gene expression. We show through simulation studies and RNA-Seq analysis of real life data that the Bayesian method yields better mapping than the current leading methods. We provide a C++ program for downloading that is being packaged into a user-friendly software. © 2011, The International Biometric Society.


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