The accessible chromatin landscape of the human genome

Robert E. Thurman; Eric Rynes; Richard Humbert; Jeff Vierstra; Matthew T. Maurano; Eric Haugen; Nathan C. Sheffield; Andrew B. Stergachis; Hao Wang; Benjamin Vernot; Kavita S. Garg; Sam John; Richard Sandstrom; Daniel Bates; Lisa Boatman; Theresa K. Canfield; Morgan Diegel; Douglas Dunn; Abigail K. Ebersol; Tristan Frum; Erika Giste; Audra Johnson; Ericka M. Johnson; Tanya Kutyavin; Bryan R. Lajoie; Bum-Kyu Lee; Kristen Lee; Darin London; Dimitra M. Lotakis; Shane Neph; Fidencio Neri; Éric Nguyen; Hongzhu Qu; Alex Reynolds; Vaughn Roach; Alexias Safi; Minerva E. Sanchez; Amartya Sanyal; Anthony Shafer; Jeremy M. Simon; Lingyun Song; Shinny Vong; Molly Weaver; Yongqi Yan; Zhancheng Zhang; Zhuzhu Zhang; Boris Lenhard; Muneesh Tewari; Michael O. Dorschner; R. Scott Hansen; Patrick A. Navas; George Stamatoyannopoulos; Vishwanath R. Iyer; Jason D. Lieb; Shamil Sunyaev; Joshua M. Akey; Peter J. Sabo; Rajinder Kaul; Terrence S. Furey; Job Dekker; Gregory E. Crawford; J Stamatoyannopoulos

doi:10.1038/nature11232

The accessible chromatin landscape of the human genome

Robert E. Thurman(Seattle University), Eric Rynes(Seattle University), Richard Humbert(Seattle University), Jeff Vierstra(Seattle University), Matthew T. Maurano(Seattle University), Eric Haugen(Seattle University), Nathan C. Sheffield(Duke University), Andrew B. Stergachis(Seattle University), Hao Wang(Seattle University), Benjamin Vernot(Seattle University), Kavita S. Garg(Cape Town HVTN Immunology Laboratory / Hutchinson Centre Research Institute of South Africa), Sam John(Seattle University), Richard Sandstrom(University of Washington), Daniel Bates(University of Washington), Lisa Boatman(Seattle University), Theresa K. Canfield(University of Washington), Morgan Diegel(University of Washington), Douglas Dunn(University of Washington), Abigail K. Ebersol(University of Washington Medical Center), Tristan Frum(University of Washington), Erika Giste(University of Washington), Audra Johnson(Seattle University), Ericka M. Johnson(University of Washington), Tanya Kutyavin(University of Washington), Bryan R. Lajoie(University of Massachusetts Chan Medical School), Bum-Kyu Lee(The University of Texas at Austin), Kristen Lee(University of Washington), Darin London(Duke University), Dimitra M. Lotakis(University of Washington Medical Center), Shane Neph(University of Washington), Fidencio Neri(Seattle University), Éric Nguyen(Seattle University), Hongzhu Qu(University of Washington), Alex Reynolds(University of Washington), Vaughn Roach(University of Washington), Alexias Safi(Duke University), Minerva E. Sanchez(University of Washington), Amartya Sanyal(University of Massachusetts Chan Medical School), Anthony Shafer(Seattle University), Jeremy M. Simon(University of North Carolina at Chapel Hill), Lingyun Song(Duke University), Shinny Vong(University of Washington), Molly Weaver(Seattle University), Yongqi Yan(University of Washington), Zhancheng Zhang(University of North Carolina at Chapel Hill), Zhuzhu Zhang(University of North Carolina at Chapel Hill), Boris Lenhard(University of Bergen), Muneesh Tewari(Fred Hutch Cancer Center), Michael O. Dorschner(University of Washington), R. Scott Hansen(University of Washington), Patrick A. Navas(University of Washington Medical Center), George Stamatoyannopoulos(University of Washington), Vishwanath R. Iyer(The University of Texas at Austin), Jason D. Lieb(University of North Carolina at Chapel Hill), Shamil Sunyaev(Harvard University), Joshua M. Akey(Seattle University), Peter J. Sabo(University of Washington), Rajinder Kaul(University of Washington Medical Center), Terrence S. Furey(University of North Carolina at Chapel Hill), Job Dekker(University of Massachusetts Chan Medical School), Gregory E. Crawford(Duke University), J Stamatoyannopoulos(Imperial College London)

Nature

September 1, 2012

10.1038/nature11232

Cited by 2,889Open Access

Full Text

Abstract

DNase I hypersensitive sites (DHSs) are markers of regulatory DNA and have underpinned the discovery of all classes of cis-regulatory elements including enhancers, promoters, insulators, silencers and locus control regions. Here we present the first extensive map of human DHSs identified through genome-wide profiling in 125 diverse cell and tissue types. We identify ∼2.9 million DHSs that encompass virtually all known experimentally validated cis-regulatory sequences and expose a vast trove of novel elements, most with highly cell-selective regulation. Annotating these elements using ENCODE data reveals novel relationships between chromatin accessibility, transcription, DNA methylation and regulatory factor occupancy patterns. We connect ∼580,000 distal DHSs with their target promoters, revealing systematic pairing of different classes of distal DHSs and specific promoter types. Patterning of chromatin accessibility at many regulatory regions is organized with dozens to hundreds of co-activated elements, and the transcellular DNase I sensitivity pattern at a given region can predict cell-type-specific functional behaviours. The DHS landscape shows signatures of recent functional evolutionary constraint. However, the DHS compartment in pluripotent and immortalized cells exhibits higher mutation rates than that in highly differentiated cells, exposing an unexpected link between chromatin accessibility, proliferative potential and patterns of human variation. An extensive map of human DNase I hypersensitive sites, markers of regulatory DNA, in 125 diverse cell and tissue types is described; integration of this information with other ENCODE-generated data sets identifies new relationships between chromatin accessibility, transcription, DNA methylation and regulatory factor occupancy patterns. This paper describes the first extensive map of human DNaseI hypersensitive sites — markers of regulatory DNA — in 125 diverse cell and tissue types. Integration of this information with other data sets generated by ENCODE (Encyclopedia of DNA Elements) identified new relationships between chromatin accessibility, transcription, DNA methylation and regulatory-factor occupancy patterns. Evolutionary-conservation analysis revealed signatures of recent functional constraint within DNaseI hypersensitive sites.

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