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LUMPY: A probabilistic framework for structural variant discovery

Comprehensive discovery of structural variation (SV) in human genomes from DNA sequencing requires the integration of multiple alignment signals including read-pair, split-read and read-depth. However, owing to inherent technical challenges, most existing SV discovery approaches utilize only one signal and consequently suffer from reduced sensitivity, especially at low sequence coverage and for smaller SVs. We present a novel and extremely flexible probabilistic SV discovery framework that is capable of integrating any number of SV detection signals including those generated from read alignments or prior evidence. We demonstrate improved sensitivity over extant methods by combining paired-end and split-read alignments and emphasize the utility of our framework for comprehensive studies of structural variation in heterogeneous tumor genomes. We further discuss the broader utility of this approach for probabilistic integration of diverse genomic interval datasets.

preprint2014arXivOpen access
Ryan M. LayerIra M. HallAaron R. Quinlan
Genomics
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Open access3 authors1 topic
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Ryan M. LayerIra M. HallAaron R. Quinlan

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