Differential use of CREB binding protein-coactivator complexes.

Riki Kurokawa,Riki Kurokawa,Riki Kurokawa,Riki Kurokawa,Christopher K Glass,Christopher K Glass,Marie-HéLèNe Ogliastro,Christopher K Glass,Marie-HéLèNe Ogliastro,Chrissa Kioussi,Daniel Kalafus,Chrissa Kioussi,Marie-HéLèNe Ogliastro,Chrissa Kioussi,Daniel Kalafus,Michael G Rosenfeld,Michael G Rosenfeld,Michael G Rosenfeld,Michael G Rosenfeld,Joseph Torchia,Joseph Torchia,Joseph Torchia,Joseph Torchia,Christopher K Glass,Chrissa Kioussi,Marie-HéLèNe Ogliastro,Daniel Kalafus,Lan Xu,Lan Xu,Lan Xu,Lan Xu,Daniel Kalafus

doi:10.1126/science.279.5351.700

Differential use of CREB binding protein-coactivator complexes.

Riki Kurokawa, Riki Kurokawa + Show 30 more

https://doi.org/10.1126/science.279.5351.700

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Journal: The Scientific monthly	Publication Date: Jan 30, 1998
Citations: 218

Affiliation: University of California, San Diego, Howard Hughes Medical Institute

#Signal Transducer And Activator Of Transcription-1 #CREB Binding Protein + Show 8 more

Abstract
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Abstract

CREB binding protein (CBP) functions as an essential coactivator of transcription factors that are inhibited by the adenovirus early gene product E1A. Transcriptional activation by the signal transducer and activator of transcription-1 (STAT1) protein requires the C/H3 domain in CBP, which is the primary target of E1A inhibition. Here it was found that the C/H3 domain is not required for retinoic acid receptor (RAR) function, nor is it involved in E1A inhibition. Instead, E1A inhibits RAR function by preventing the assembly of CBP-nuclear receptor coactivator complexes, revealing differences in required CBP domains for transcriptional activation by RAR and STAT1.

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