Nucleosome dynamics define transcriptional enhancers

Housheng Hansen He; Clifford A. Meyer; Hyunjin Shin; Shannon T. Bailey; Gang Wei; Qianben Wang; Yong Zhang; Kexin Xu; Min Ni; Mathieu Lupien; Piotr Mieczkowski; Jason D. Lieb; Keji Zhao; Myles Brown; X. Shirley Liu

doi:10.1038/ng.545

Nucleosome dynamics define transcriptional enhancers

Housheng Hansen He
, Clifford A. Meyer
, Hyunjin Shin
, Shannon T. Bailey
, Gang Wei
, Qianben Wang
, Yong Zhang
, Kexin Xu
, Min Ni
, Mathieu Lupien
, Piotr Mieczkowski
, Jason D. Lieb
, Keji Zhao
, Myles Brown
, X. Shirley Liu

Producción científica: Article › revisión exhaustiva

401 Citas (Scopus)

Resumen

Chromatin plays a central role in eukaryotic gene regulation. We performed genome-wide mapping of epigenetically marked nucleosomes to determine their position both near transcription start sites and at distal regulatory elements, including enhancers. In prostate cancer cells, where androgen receptor binds primarily to enhancers, we found that androgen treatment dismisses a central nucleosome present at androgen receptor binding sites that is flanked by a pair of marked nucleosomes. A new quantitative model built on the behavior of such nucleosome pairs correctly identified regions bound by the regulators of the immediate androgen response, including androgen receptor and FOXA1. More importantly, this model also correctly predicted previously unidentified binding sites for other transcription factors present after prolonged androgen stimulation, including OCT1 and NKX3-1. Therefore, quantitative modeling of enhancer structure provides a powerful predictive method to infer the identity of transcription factors involved in cellular responses to specific stimuli.

Idioma original	English (US)
Páginas (desde-hasta)	343-347
Número de páginas	5
Publicación	Nature Genetics
Volumen	42
N.º	4
DOI	https://doi.org/10.1038/ng.545
Estado	Published - abr 2010
Publicado de forma externa	Sí

ASJC Scopus subject areas

Genetics

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@article{56cbd453481c474e81398c7664e7e24e,

title = "Nucleosome dynamics define transcriptional enhancers",

abstract = "Chromatin plays a central role in eukaryotic gene regulation. We performed genome-wide mapping of epigenetically marked nucleosomes to determine their position both near transcription start sites and at distal regulatory elements, including enhancers. In prostate cancer cells, where androgen receptor binds primarily to enhancers, we found that androgen treatment dismisses a central nucleosome present at androgen receptor binding sites that is flanked by a pair of marked nucleosomes. A new quantitative model built on the behavior of such nucleosome pairs correctly identified regions bound by the regulators of the immediate androgen response, including androgen receptor and FOXA1. More importantly, this model also correctly predicted previously unidentified binding sites for other transcription factors present after prolonged androgen stimulation, including OCT1 and NKX3-1. Therefore, quantitative modeling of enhancer structure provides a powerful predictive method to infer the identity of transcription factors involved in cellular responses to specific stimuli.",

author = "He, \{Housheng Hansen\} and Meyer, \{Clifford A.\} and Hyunjin Shin and Bailey, \{Shannon T.\} and Gang Wei and Qianben Wang and Yong Zhang and Kexin Xu and Min Ni and Mathieu Lupien and Piotr Mieczkowski and Lieb, \{Jason D.\} and Keji Zhao and Myles Brown and Liu, \{X. Shirley\}",

note = "Funding Information: This work was supported by grants from US National Institutes of Health (1R01 HG004069-02 to X.S.L., and 2P50 CA090381-06 to X.S.L. and M.B.), the Department of Defense (W81XWH-07-1-0037 to X.S.L.) and the Prostate Cancer Foundation (to M.B.).",

year = "2010",

month = apr,

doi = "10.1038/ng.545",

language = "English (US)",

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AU - He, Housheng Hansen

AU - Meyer, Clifford A.

AU - Shin, Hyunjin

AU - Bailey, Shannon T.

AU - Wei, Gang

AU - Wang, Qianben

AU - Zhang, Yong

AU - Xu, Kexin

AU - Ni, Min

AU - Lupien, Mathieu

AU - Mieczkowski, Piotr

AU - Lieb, Jason D.

AU - Zhao, Keji

AU - Brown, Myles

AU - Liu, X. Shirley

N1 - Funding Information: This work was supported by grants from US National Institutes of Health (1R01 HG004069-02 to X.S.L., and 2P50 CA090381-06 to X.S.L. and M.B.), the Department of Defense (W81XWH-07-1-0037 to X.S.L.) and the Prostate Cancer Foundation (to M.B.).

PY - 2010/4

Y1 - 2010/4

N2 - Chromatin plays a central role in eukaryotic gene regulation. We performed genome-wide mapping of epigenetically marked nucleosomes to determine their position both near transcription start sites and at distal regulatory elements, including enhancers. In prostate cancer cells, where androgen receptor binds primarily to enhancers, we found that androgen treatment dismisses a central nucleosome present at androgen receptor binding sites that is flanked by a pair of marked nucleosomes. A new quantitative model built on the behavior of such nucleosome pairs correctly identified regions bound by the regulators of the immediate androgen response, including androgen receptor and FOXA1. More importantly, this model also correctly predicted previously unidentified binding sites for other transcription factors present after prolonged androgen stimulation, including OCT1 and NKX3-1. Therefore, quantitative modeling of enhancer structure provides a powerful predictive method to infer the identity of transcription factors involved in cellular responses to specific stimuli.

AB - Chromatin plays a central role in eukaryotic gene regulation. We performed genome-wide mapping of epigenetically marked nucleosomes to determine their position both near transcription start sites and at distal regulatory elements, including enhancers. In prostate cancer cells, where androgen receptor binds primarily to enhancers, we found that androgen treatment dismisses a central nucleosome present at androgen receptor binding sites that is flanked by a pair of marked nucleosomes. A new quantitative model built on the behavior of such nucleosome pairs correctly identified regions bound by the regulators of the immediate androgen response, including androgen receptor and FOXA1. More importantly, this model also correctly predicted previously unidentified binding sites for other transcription factors present after prolonged androgen stimulation, including OCT1 and NKX3-1. Therefore, quantitative modeling of enhancer structure provides a powerful predictive method to infer the identity of transcription factors involved in cellular responses to specific stimuli.

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Nucleosome dynamics define transcriptional enhancers

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