Breast cancer associated transcriptional repressor PLU-1/JARID1B interacts directly with histone deacetylases

A Barrett; S Santangelo; K Tan; S Catchpole; K Roberts; B Spencer-Dene; D Hall; A Scibetta; J Burchell; E Verdin; P Freemont; J Taylor-Papadimitriou

doi:10.1002/ijc.22673

Breast cancer associated transcriptional repressor PLU-1/JARID1B interacts directly with histone deacetylases

A Barrett, S Santangelo, K Tan, S Catchpole, K Roberts, B Spencer-Dene, D Hall, A Scibetta, J Burchell, E Verdin, P Freemont, J Taylor-Papadimitriou

Comprehensive Cancer Centre

Research output: Contribution to journal › Article › peer-review

83 Citations (Scopus)

Abstract

The PLU-1/JARID1B nuclear protein, which is expressed in a high proportion of breast cancers, but shows restricted expression elsewhere, belongs to the ARID family of proteins, known to play important roles in development, differentiation, transcriptional regulation and chromatin remodeling. PLU-1/JARID1B is a strong transcriptional repressor, and here we show that the protein localizes in MAD bodies when cotransfected with class IIa histone deacetylases (HDACs) or N-CoR. Direct binding to class I and class IIa HDACs is demonstrated, while the interaction with N-CoR appears to be indirect. The domains involved in the HDAC4-PLU-1/JARID1B interaction were investigated in detail, and the data show that 2 PHD domains in PLU-1/JARID1B, which are involved in transcriptional repression, are also crucial for binding to a domain in the 5' region of HDAC4, overlapping the MEF-2 binding region. Physiological relevance of this interaction in the mammary gland is suggested from the observation that HDAC4 and PLU-1/JARID1B are coexpressed in the pregnant and involuting mouse mammary gland and are both silenced at lactation. Significantly, the expression of both proteins is seen in breast cancers. (c) 2007 Wiley-Liss, lnc

Original language	English
Pages (from-to)	265 - 275
Number of pages	11
Journal	International Journal of Cancer
Volume	121
Issue number	2
DOIs	https://doi.org/10.1002/ijc.22673
Publication status	Published - 15 Jul 2007

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Barrett, A., Santangelo, S., Tan, K., Catchpole, S., Roberts, K., Spencer-Dene, B., Hall, D., Scibetta, A., Burchell, J., Verdin, E., Freemont, P., & Taylor-Papadimitriou, J. (2007). Breast cancer associated transcriptional repressor PLU-1/JARID1B interacts directly with histone deacetylases. International Journal of Cancer, 121(2), 265 - 275. https://doi.org/10.1002/ijc.22673

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title = "Breast cancer associated transcriptional repressor PLU-1/JARID1B interacts directly with histone deacetylases",

abstract = "The PLU-1/JARID1B nuclear protein, which is expressed in a high proportion of breast cancers, but shows restricted expression elsewhere, belongs to the ARID family of proteins, known to play important roles in development, differentiation, transcriptional regulation and chromatin remodeling. PLU-1/JARID1B is a strong transcriptional repressor, and here we show that the protein localizes in MAD bodies when cotransfected with class IIa histone deacetylases (HDACs) or N-CoR. Direct binding to class I and class IIa HDACs is demonstrated, while the interaction with N-CoR appears to be indirect. The domains involved in the HDAC4-PLU-1/JARID1B interaction were investigated in detail, and the data show that 2 PHD domains in PLU-1/JARID1B, which are involved in transcriptional repression, are also crucial for binding to a domain in the 5' region of HDAC4, overlapping the MEF-2 binding region. Physiological relevance of this interaction in the mammary gland is suggested from the observation that HDAC4 and PLU-1/JARID1B are coexpressed in the pregnant and involuting mouse mammary gland and are both silenced at lactation. Significantly, the expression of both proteins is seen in breast cancers. (c) 2007 Wiley-Liss, lnc",

author = "A Barrett and S Santangelo and K Tan and S Catchpole and K Roberts and B Spencer-Dene and D Hall and A Scibetta and J Burchell and E Verdin and P Freemont and J Taylor-Papadimitriou",

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Barrett, A, Santangelo, S, Tan, K, Catchpole, S, Roberts, K, Spencer-Dene, B, Hall, D, Scibetta, A, Burchell, J, Verdin, E, Freemont, P & Taylor-Papadimitriou, J 2007, 'Breast cancer associated transcriptional repressor PLU-1/JARID1B interacts directly with histone deacetylases', International Journal of Cancer, vol. 121, no. 2, pp. 265 - 275. https://doi.org/10.1002/ijc.22673

TY - JOUR

T1 - Breast cancer associated transcriptional repressor PLU-1/JARID1B interacts directly with histone deacetylases

AU - Barrett, A

AU - Santangelo, S

AU - Tan, K

AU - Catchpole, S

AU - Roberts, K

AU - Spencer-Dene, B

AU - Hall, D

AU - Scibetta, A

AU - Burchell, J

AU - Verdin, E

AU - Freemont, P

AU - Taylor-Papadimitriou, J

PY - 2007/7/15

Y1 - 2007/7/15

N2 - The PLU-1/JARID1B nuclear protein, which is expressed in a high proportion of breast cancers, but shows restricted expression elsewhere, belongs to the ARID family of proteins, known to play important roles in development, differentiation, transcriptional regulation and chromatin remodeling. PLU-1/JARID1B is a strong transcriptional repressor, and here we show that the protein localizes in MAD bodies when cotransfected with class IIa histone deacetylases (HDACs) or N-CoR. Direct binding to class I and class IIa HDACs is demonstrated, while the interaction with N-CoR appears to be indirect. The domains involved in the HDAC4-PLU-1/JARID1B interaction were investigated in detail, and the data show that 2 PHD domains in PLU-1/JARID1B, which are involved in transcriptional repression, are also crucial for binding to a domain in the 5' region of HDAC4, overlapping the MEF-2 binding region. Physiological relevance of this interaction in the mammary gland is suggested from the observation that HDAC4 and PLU-1/JARID1B are coexpressed in the pregnant and involuting mouse mammary gland and are both silenced at lactation. Significantly, the expression of both proteins is seen in breast cancers. (c) 2007 Wiley-Liss, lnc

AB - The PLU-1/JARID1B nuclear protein, which is expressed in a high proportion of breast cancers, but shows restricted expression elsewhere, belongs to the ARID family of proteins, known to play important roles in development, differentiation, transcriptional regulation and chromatin remodeling. PLU-1/JARID1B is a strong transcriptional repressor, and here we show that the protein localizes in MAD bodies when cotransfected with class IIa histone deacetylases (HDACs) or N-CoR. Direct binding to class I and class IIa HDACs is demonstrated, while the interaction with N-CoR appears to be indirect. The domains involved in the HDAC4-PLU-1/JARID1B interaction were investigated in detail, and the data show that 2 PHD domains in PLU-1/JARID1B, which are involved in transcriptional repression, are also crucial for binding to a domain in the 5' region of HDAC4, overlapping the MEF-2 binding region. Physiological relevance of this interaction in the mammary gland is suggested from the observation that HDAC4 and PLU-1/JARID1B are coexpressed in the pregnant and involuting mouse mammary gland and are both silenced at lactation. Significantly, the expression of both proteins is seen in breast cancers. (c) 2007 Wiley-Liss, lnc

U2 - 10.1002/ijc.22673

DO - 10.1002/ijc.22673

M3 - Article

SN - 1097-0215

VL - 121

SP - 265

EP - 275

JO - International Journal of Cancer

JF - International Journal of Cancer

IS - 2

ER -

Breast cancer associated transcriptional repressor PLU-1/JARID1B interacts directly with histone deacetylases

Abstract

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