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      Accurate inference of transcription factor binding from DNA sequence and chromatin accessibility data.

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          Abstract

          Accurate functional annotation of regulatory elements is essential for understanding global gene regulation. Here, we report a genome-wide map of 827,000 transcription factor binding sites in human lymphoblastoid cell lines, which is comprised of sites corresponding to 239 position weight matrices of known transcription factor binding motifs, and 49 novel sequence motifs. To generate this map, we developed a probabilistic framework that integrates cell- or tissue-specific experimental data such as histone modifications and DNase I cleavage patterns with genomic information such as gene annotation and evolutionary conservation. Comparison to empirical ChIP-seq data suggests that our method is highly accurate yet has the advantage of targeting many factors in a single assay. We anticipate that this approach will be a valuable tool for genome-wide studies of gene regulation in a wide variety of cell types or tissues under diverse conditions.

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          Author and article information

          Journal
          Genome Res
          Genome research
          Cold Spring Harbor Laboratory
          1549-5469
          1088-9051
          Mar 2011
          : 21
          : 3
          Affiliations
          [1 ] Department of Human Genetics, University of Chicago, Chicago, Illinois 60637, USA. rpique@uchicago.edu
          Article
          gr.112623.110
          10.1101/gr.112623.110
          3044858
          21106904
          0f022fde-1f1d-4d70-9e1c-014b6a47c6d3
          History

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