Publication | Open Access
Chromatin segmentation based on a probabilistic model for read counts explains a large portion of the epigenome
96
Citations
17
References
2015
Year
Histone ModificationsEngineeringEpigenetic ChangeGeneticsLarge PortionGenomicsEpigeneticsComputational GenomicsBiostatisticsChromatin SegmentationChromatin BiologyNuclear OrganizationModification MapsBioinformaticsFunctional GenomicsChromatinRead CountsChromatin RemodelingGene Sequence AnnotationComputational BiologyEpigenomicsSystems BiologyMedicineChromatin ImmunoprecipitationGenome Editing
Chromatin immunoprecipitation followed by sequencing (ChIP-seq) is an increasingly common experimental approach to generate genome-wide maps of histone modifications and to dissect the complexity of the epigenome. Here, we propose EpiCSeg: a novel algorithm that combines several histone modification maps for the segmentation and characterization of cell-type specific epigenomic landscapes. By using an accurate probabilistic model for the read counts, EpiCSeg provides a useful annotation for a considerably larger portion of the genome, shows a stronger association with validation data, and yields more consistent predictions across replicate experiments when compared to existing methods.The software is available at http://github.com/lamortenera/epicseg.
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