Agonist and antagonist switch DNA motifs recognized by human androgen receptor in prostate cancer

Zhong Chen; Xun Lan; Jennifer M. Thomas-Ahner; Dayong Wu; Xiangtao Liu; Zhenqing Ye; Liguo Wang; Benjamin Sunkel; Cassandra Grenade; Junsheng Chen; Debra L. Zynger; Pearlly S. Yan; Jiaoti Huang; Kenneth P. Nephew; Tim H.M. Huang; Shili Lin; Steven K. Clinton; Wei Li; Victor X. Jin; Qianben Wang

doi:10.15252/embj.201490306

Agonist and antagonist switch DNA motifs recognized by human androgen receptor in prostate cancer

Zhong Chen, Xun Lan, Jennifer M. Thomas-Ahner, Dayong Wu, Xiangtao Liu, Zhenqing Ye, Liguo Wang, Benjamin Sunkel, Cassandra Grenade, Junsheng Chen, Debra L. Zynger, Pearlly S. Yan, Jiaoti Huang, Kenneth P. Nephew, Tim H.M. Huang, Shili Lin, Steven K. Clinton, Wei Li, Victor X. Jin, Qianben Wang

Department of Molecular Medicine

Producción científica: Article › revisión exhaustiva

72 Citas (Scopus)

Resumen

Human transcription factors recognize specific DNA sequence motifs to regulate transcription. It is unknown whether a single transcription factor is able to bind to distinctly different motifs on chromatin, and if so, what determines the usage of specific motifs. By using a motif-resolution chromatin immunoprecipitationexonuclease (ChIP-exo) approach, we find that agonist-liganded human androgen receptor (AR) and antagonist-liganded AR bind to two distinctly different motifs, leading to distinct transcriptional outcomes in prostate cancer cells. Further analysis on clinical prostate tissues reveals that the binding of AR to these two distinct motifs is involved in prostate carcinogenesis. Together, these results suggest that unique ligands may switch DNA motifs recognized by ligand-dependent transcription factors in vivo. Our findings also provide a broad mechanistic foundation for understanding ligand-specific induction of gene expression profiles.

Idioma original	English (US)
Páginas (desde-hasta)	502-516
Número de páginas	15
Publicación	EMBO Journal
Volumen	34
N.º	4
DOI	https://doi.org/10.15252/embj.201490306
Estado	Published - feb 12 2015

ASJC Scopus subject areas

General Neuroscience
Molecular Biology
General Biochemistry, Genetics and Molecular Biology
General Immunology and Microbiology

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10.15252/embj.201490306

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Chen, Z., Lan, X., Thomas-Ahner, J. M., Wu, D., Liu, X., Ye, Z., Wang, L., Sunkel, B., Grenade, C., Chen, J., Zynger, D. L., Yan, P. S., Huang, J., Nephew, K. P., Huang, T. H. M., Lin, S., Clinton, S. K., Li, W., Jin, V. X., & Wang, Q. (2015). Agonist and antagonist switch DNA motifs recognized by human androgen receptor in prostate cancer. EMBO Journal, 34(4), 502-516. https://doi.org/10.15252/embj.201490306

Chen, Z, Lan, X, Thomas-Ahner, JM, Wu, D, Liu, X, Ye, Z, Wang, L, Sunkel, B, Grenade, C, Chen, J, Zynger, DL, Yan, PS, Huang, J, Nephew, KP, Huang, THM, Lin, S, Clinton, SK, Li, W, Jin, VX & Wang, Q 2015, 'Agonist and antagonist switch DNA motifs recognized by human androgen receptor in prostate cancer', EMBO Journal, vol. 34, n.º 4, pp. 502-516. https://doi.org/10.15252/embj.201490306

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title = "Agonist and antagonist switch DNA motifs recognized by human androgen receptor in prostate cancer",

abstract = "Human transcription factors recognize specific DNA sequence motifs to regulate transcription. It is unknown whether a single transcription factor is able to bind to distinctly different motifs on chromatin, and if so, what determines the usage of specific motifs. By using a motif-resolution chromatin immunoprecipitationexonuclease (ChIP-exo) approach, we find that agonist-liganded human androgen receptor (AR) and antagonist-liganded AR bind to two distinctly different motifs, leading to distinct transcriptional outcomes in prostate cancer cells. Further analysis on clinical prostate tissues reveals that the binding of AR to these two distinct motifs is involved in prostate carcinogenesis. Together, these results suggest that unique ligands may switch DNA motifs recognized by ligand-dependent transcription factors in vivo. Our findings also provide a broad mechanistic foundation for understanding ligand-specific induction of gene expression profiles.",

keywords = "Androgen receptor, ChIP-exo, DNA motif switching, Prostate cancer, Transcription factor",

author = "Zhong Chen and Xun Lan and Thomas-Ahner, {Jennifer M.} and Dayong Wu and Xiangtao Liu and Zhenqing Ye and Liguo Wang and Benjamin Sunkel and Cassandra Grenade and Junsheng Chen and Zynger, {Debra L.} and Yan, {Pearlly S.} and Jiaoti Huang and Nephew, {Kenneth P.} and Huang, {Tim H.M.} and Shili Lin and Clinton, {Steven K.} and Wei Li and Jin, {Victor X.} and Qianben Wang",

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doi = "10.15252/embj.201490306",

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AU - Chen, Zhong

AU - Lan, Xun

AU - Thomas-Ahner, Jennifer M.

AU - Wu, Dayong

AU - Liu, Xiangtao

AU - Ye, Zhenqing

AU - Wang, Liguo

AU - Sunkel, Benjamin

AU - Grenade, Cassandra

AU - Chen, Junsheng

AU - Zynger, Debra L.

AU - Yan, Pearlly S.

AU - Huang, Jiaoti

AU - Nephew, Kenneth P.

AU - Huang, Tim H.M.

AU - Lin, Shili

AU - Clinton, Steven K.

AU - Li, Wei

AU - Jin, Victor X.

AU - Wang, Qianben

PY - 2015/2/12

Y1 - 2015/2/12

N2 - Human transcription factors recognize specific DNA sequence motifs to regulate transcription. It is unknown whether a single transcription factor is able to bind to distinctly different motifs on chromatin, and if so, what determines the usage of specific motifs. By using a motif-resolution chromatin immunoprecipitationexonuclease (ChIP-exo) approach, we find that agonist-liganded human androgen receptor (AR) and antagonist-liganded AR bind to two distinctly different motifs, leading to distinct transcriptional outcomes in prostate cancer cells. Further analysis on clinical prostate tissues reveals that the binding of AR to these two distinct motifs is involved in prostate carcinogenesis. Together, these results suggest that unique ligands may switch DNA motifs recognized by ligand-dependent transcription factors in vivo. Our findings also provide a broad mechanistic foundation for understanding ligand-specific induction of gene expression profiles.

AB - Human transcription factors recognize specific DNA sequence motifs to regulate transcription. It is unknown whether a single transcription factor is able to bind to distinctly different motifs on chromatin, and if so, what determines the usage of specific motifs. By using a motif-resolution chromatin immunoprecipitationexonuclease (ChIP-exo) approach, we find that agonist-liganded human androgen receptor (AR) and antagonist-liganded AR bind to two distinctly different motifs, leading to distinct transcriptional outcomes in prostate cancer cells. Further analysis on clinical prostate tissues reveals that the binding of AR to these two distinct motifs is involved in prostate carcinogenesis. Together, these results suggest that unique ligands may switch DNA motifs recognized by ligand-dependent transcription factors in vivo. Our findings also provide a broad mechanistic foundation for understanding ligand-specific induction of gene expression profiles.

KW - Androgen receptor

KW - ChIP-exo

KW - DNA motif switching

KW - Prostate cancer

KW - Transcription factor

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Agonist and antagonist switch DNA motifs recognized by human androgen receptor in prostate cancer

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ASJC Scopus subject areas

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