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Dynamics of the Epigenetic Landscape During Erythroid Differentiation after Gata1 Restoration

Authors :
Massachusetts Institute of Technology. Computer Science and Artificial Intelligence Laboratory
Kellis, Manolis
Ernst, Jason
Wu, Weisheng
Cheng, Yong
Keller, Cheryl A.
Kumar, Swathi Ashok
Mishra, Tejaswini
Morrissey, Christapher
Dorman, Christine M.
Chen, Kuan-Bei
Drautz, Daniela
Giardine, Belinda
Shibata, Yoichiro
Song, Lingyun
Pimkin, Max
Crawford, Gregory E.
Furey, Terrence S.
Miller, Webb
Taylor, James
Schuster, Stephan C.
Zhang, Yu
Chiaromonte, Francesca
Blobel, Gerd A.
Weiss, Mitchell J.
Hardison, Ross C.
Massachusetts Institute of Technology. Computer Science and Artificial Intelligence Laboratory
Kellis, Manolis
Ernst, Jason
Wu, Weisheng
Cheng, Yong
Keller, Cheryl A.
Kumar, Swathi Ashok
Mishra, Tejaswini
Morrissey, Christapher
Dorman, Christine M.
Chen, Kuan-Bei
Drautz, Daniela
Giardine, Belinda
Shibata, Yoichiro
Song, Lingyun
Pimkin, Max
Crawford, Gregory E.
Furey, Terrence S.
Miller, Webb
Taylor, James
Schuster, Stephan C.
Zhang, Yu
Chiaromonte, Francesca
Blobel, Gerd A.
Weiss, Mitchell J.
Hardison, Ross C.
Source :
Genome Research
Publication Year :
2012

Abstract

Interplays among lineage-specific nuclear proteins, chromatin modifying enzymes, and the basal transcription machinery govern cellular differentiation, but their dynamics of action and coordination with transcriptional control are not fully understood. Alterations in chromatin structure appear to establish a permissive state for gene activation at some loci, but they play an integral role in activation at other loci. To determine the predominant roles of chromatin states and factor occupancy in directing gene regulation during differentiation, we mapped chromatin accessibility, histone modifications, and nuclear factor occupancy genome-wide during mouse erythroid differentiation dependent on the master regulatory transcription factor GATA1. Notably, despite extensive changes in gene expression, the chromatin state profiles (proportions of a gene in a chromatin state dominated by activating or repressive histone modifications) and accessibility remain largely unchanged during GATA1-induced erythroid differentiation. In contrast, gene induction and repression are strongly associated with changes in patterns of transcription factor occupancy. Our results indicate that during erythroid differentiation, the broad features of chromatin states are established at the stage of lineage commitment, largely independently of GATA1. These determine permissiveness for expression, with subsequent induction or repression mediated by distinctive combinations of transcription factors<br />National Institutes of Health (U.S.) (Grant number RC1HG005334)<br />National Science Foundation (U.S.). (Award 0905968)

Details

Database :
OAIster
Journal :
Genome Research
Notes :
application/pdf, en_US
Publication Type :
Electronic Resource
Accession number :
edsoai.ocn812036473
Document Type :
Electronic Resource