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Integrating Diverse Datasets Improves Developmental Enhancer Prediction
Authors
A Arvey
A Barski
+109 more
A Ben-Hur
A He
A Miquelajauregui
A Rada-Iglesias
A Siepel
A Visel
A Visel
A Visel
A Visel
A Visel
A Visel
A Woolfe
A Woznica
AI Su
AP Boyle
AR Quinlan
AS Nord
BW Busser
C Cheng
C Jin
C Leslie
CE Grant
CM Koch
CT Ong
CY McLean
D Lee
D May
D Wang
Dennis Kostka
DM McGaughey
DS Johnson
DU Gorkin
E Birney
E Seuntjens
G Cuellar-Partida
GE Zentner
Genevieve D. Erwin
GM Burzynski
H Lahdesmaki
HH He
I Dunham
J Banerji
J Cotney
J Ernst
JA Capra
JA Capra
JA Wamstad
John A. Capra
JP Noonan
K Koshiba-Takeuchi
K Lindblad-Toh
KA Aldinger
Karl K. Murphy
Katherine S. Pollard
KJ Won
KS Pollard
KY Yip
L Narlikar
L Taher
LA Hindorff
LA Pennacchio
M Bulger
M Kloft
M Levine
M Wilson
MA Nobrega
MA White
MJ Blow
MM El-Kasti
MM Hoffman
MP Creyghton
MR Kantorovitz
N Oksenberg
N Rajagopal
Nadav Ahituv
ND Heintzman
ND Heintzman
NE Renthal
Nir Oksenberg
NJ Sakabe
PG Giresi
Q Li
Q Weng
R Andersson
R O'Rahilly
R Pique-Regi
RE Thurman
Rebecca M. Truty
RP Zinzen
RS Smith
S Bonn
S Ghisletti
S Lomvardas
S Prabhakar
S Salzberg
S Sonnenburg
S Sonnenburg
SD Gillies
SJ Sholtis
SL Paige
T Casci
T Kume
T Kume
TG Dietterich
TS Mikkelsen
UA Orom
Uwe Ohler
VW Zhou
Z Wang
Publication date
27 September 2013
Publisher
'Public Library of Science (PLoS)'
Doi
View
on
arXiv
Abstract
Gene-regulatory enhancers have been identified using various approaches, including evolutionary conservation, regulatory protein binding, chromatin modifications, and DNA sequence motifs. To integrate these different approaches, we developed EnhancerFinder, a two-step method for distinguishing developmental enhancers from the genomic background and then predicting their tissue specificity. EnhancerFinder uses a multiple kernel learning approach to integrate DNA sequence motifs, evolutionary patterns, and diverse functional genomics datasets from a variety of cell types. In contrast with prediction approaches that define enhancers based on histone marks or p300 sites from a single cell line, we trained EnhancerFinder on hundreds of experimentally verified human developmental enhancers from the VISTA Enhancer Browser. We comprehensively evaluated EnhancerFinder using cross validation and found that our integrative method improves the identification of enhancers over approaches that consider a single type of data, such as sequence motifs, evolutionary conservation, or the binding of enhancer-associated proteins. We find that VISTA enhancers active in embryonic heart are easier to identify than enhancers active in several other embryonic tissues, likely due to their uniquely high GC content. We applied EnhancerFinder to the entire human genome and predicted 84,301 developmental enhancers and their tissue specificity. These predictions provide specific functional annotations for large amounts of human non-coding DNA, and are significantly enriched near genes with annotated roles in their predicted tissues and lead SNPs from genome-wide association studies. We demonstrate the utility of EnhancerFinder predictions through in vivo validation of novel embryonic gene regulatory enhancers from three developmental transcription factor loci. Our genome-wide developmental enhancer predictions are freely available as a UCSC Genome Browser track, which we hope will enable researchers to further investigate questions in developmental biology. © 2014 Erwin et al
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