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High Resolution Genome Wide Binding Event Finding and Motif Discovery Reveals Transcription Factor Spatial Binding Constraints

Overview of attention for article published in PLoS Computational Biology, August 2012
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Title
High Resolution Genome Wide Binding Event Finding and Motif Discovery Reveals Transcription Factor Spatial Binding Constraints
Published in
PLoS Computational Biology, August 2012
DOI 10.1371/journal.pcbi.1002638
Pubmed ID
Authors

Yuchun Guo, Shaun Mahony, David K. Gifford

Abstract

An essential component of genome function is the syntax of genomic regulatory elements that determine how diverse transcription factors interact to orchestrate a program of regulatory control. A precise characterization of in vivo spacing constraints between key transcription factors would reveal key aspects of this genomic regulatory language. To discover novel transcription factor spatial binding constraints in vivo, we developed a new integrative computational method, genome wide event finding and motif discovery (GEM). GEM resolves ChIP data into explanatory motifs and binding events at high spatial resolution by linking binding event discovery and motif discovery with positional priors in the context of a generative probabilistic model of ChIP data and genome sequence. GEM analysis of 63 transcription factors in 214 ENCODE human ChIP-Seq experiments recovers more known factor motifs than other contemporary methods, and discovers six new motifs for factors with unknown binding specificity. GEM's adaptive learning of binding-event read distributions allows it to further improve upon previous methods for processing ChIP-Seq and ChIP-exo data to yield unsurpassed spatial resolution and discovery of closely spaced binding events of the same factor. In a systematic analysis of in vivo sequence-specific transcription factor binding using GEM, we have found hundreds of spatial binding constraints between factors. GEM found 37 examples of factor binding constraints in mouse ES cells, including strong distance-specific constraints between Klf4 and other key regulatory factors. In human ENCODE data, GEM found 390 examples of spatially constrained pair-wise binding, including such novel pairs as c-Fos:c-Jun/USF1, CTCF/Egr1, and HNF4A/FOXA1. The discovery of new factor-factor spatial constraints in ChIP data is significant because it proposes testable models for regulatory factor interactions that will help elucidate genome function and the implementation of combinatorial control.

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Mendeley readers

The data shown below were compiled from readership statistics for 334 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
United States 12 4%
United Kingdom 5 1%
Netherlands 2 <1%
France 2 <1%
India 2 <1%
Austria 1 <1%
Australia 1 <1%
Italy 1 <1%
Portugal 1 <1%
Other 7 2%
Unknown 300 90%

Demographic breakdown

Readers by professional status Count As %
Student > Ph. D. Student 110 33%
Researcher 77 23%
Student > Master 33 10%
Student > Bachelor 28 8%
Professor > Associate Professor 16 5%
Other 41 12%
Unknown 29 9%
Readers by discipline Count As %
Agricultural and Biological Sciences 163 49%
Biochemistry, Genetics and Molecular Biology 75 22%
Computer Science 27 8%
Medicine and Dentistry 10 3%
Mathematics 4 1%
Other 17 5%
Unknown 38 11%