A Novel Corepressor, BCoR-L1, Represses Transcription Through an Interaction with CtBP

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K. Pagan, Julia
Arnold, Jeremy
J. Hanchard, Kim
Kumar, Raman
Bruno, Tiziana
J. K. Jones, Mathew
J. Richard, Derek
Forrest, Alistair
Spurdle, Amanda
Verdin, Eric
Crossley, Merlin
Fanciulli, Maurizio
Chenevix-Trench, Georgia
B. Young, David
Khanna, Kum Kum
Griffith University Author(s)
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2007
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Abstract

Corepressors play a crucial role in negative gene regulation and are defective in several diseases. BCoR is a corepressor for the BCL6 repressor protein. Here we describe and functionally characterize BCoR-L1, a homolog of BCoR. When tethered to a heterologous promoter, BCoR-L1 is capable of strong repression. Like other corepressors, BCoR-L1 associates with histone deacetylase (HDAC) activity. Specifically, BCoR-L1 coprecipitates with the Class II HDACs, HDAC4, HDAC5, and HDAC7, suggesting that they are involved in its role as a transcriptional repressor. BCoR-L1 also interacts with the CtBP corepressor through a CtBP-interacting motif in its amino terminus. Abrogation of the CtBP binding site within BCoR-L1 partially relieves BCoR-L1-mediated transcriptional repression. Furthermore, BCoR-L1 is located on the E-cadherin promoter, a known CtBP-regulated promoter, and represses the E-cadherin promoter activity in a reporter assay. The inhibition of BCoR-L1 expression by RNA-mediated interference results in derepression of E-cadherin in cells that do not normally express E-cadherin, indicating that BCoR-L1 contributes to the repression of an authentic endogenous CtBP target.

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Journal of Biological Chemistry

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282

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20

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Chemical Sciences

Biological Sciences

Medical and Health Sciences

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