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High-resolution genome-wide in vivo footprinting of diverse transcription factors in human cells

  • Alan P. Boyle
  • , Lingyun Song
  • , Bum Kyu Lee
  • , Darin London
  • , Damian Keefe
  • , Ewan Birney
  • , Vishwanath R. Iyer
  • , Gregory E. Crawford
  • , Terrence S. Furey
  • Duke University
  • European Molecular Biology Laboratory
  • University of Texas at Austin

Research output: Contribution to journalArticlepeer-review

268 Scopus citations

Abstract

Regulation of gene transcription in diverse cell types is determined largely by varied sets of cis-elements where transcription factors bind. Here we demonstrate that data from a single high-throughput DNase I hypersensitivity assay can delineate hundreds of thousands of base-pair resolution in vivo footprints in human cells that precisely mark individual transcription factor-DNA interactions. These annotations provide a unique resource for the investigation of cis-regulatory elements. We find that footprints for specific transcription factors correlate with ChIP-seq enrichment and can accurately identify functional versus nonfunctional transcription factor motifs. We also find that footprints reveal a unique evolutionary conservation pattern that differentiates functional footprinted bases from surrounding DNA. Finally, detailed analysis of CTCF footprints suggests multiple modes of binding and a novel DNA binding motif upstream of the primary binding site.

Original languageEnglish
Pages (from-to)456-464
Number of pages9
JournalGenome Research
Volume21
Issue number3
DOIs
StatePublished - Mar 2011

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