Detection of copy number variation from array intensity and sequencing read depth using a stepwise Bayesian model

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Background: Copy number variants (CNVs) have been demonstrated to occur at a high frequency and are now widely believed to make a significant contribution to the phenotypic variation in human populations. Array-based comparative genomic hybridization (array-CGH) and newly developed read-depth approach through ultrahigh throughput genomic sequencing both provide rapid, robust, and comprehensive methods to identify CNVs on a whole-genome scale. Results: We developed a Bayesian statistical analysis algorithm for the detection of CNVs from both types of genomic data. The algorithm can analyze such data obtained from PCR-based bacterial artificial chromosome arrays, high-density oligonucleotide arrays, and more recently developed high-throughput DNA sequencing. Treating parameters

Zhengdong D. Zhang, Mark B. Gerstein

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BMCBI 2010 | Comparative Genomic Hybridization | Genomic | Posterior Distribution |

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Added	08 Dec 2010
Updated	08 Dec 2010
Type	Journal
Year	2010
Where	BMCBI
Authors	Zhengdong D. Zhang, Mark B. Gerstein

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Detection of copy number variation from array intensity and sequencing read depth using a stepwise Bayesian model

BMCBI 2010 | Comparative Genomic Hybridization | Genomic | Posterior Distribution |

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