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Genome-wide analysis of cAMP-response element binding protein occupancy, phosphorylation, and target gene activation in human tissues.


ABSTRACT: Hormones and nutrients often induce genetic programs via signaling pathways that interface with gene-specific activators. Activation of the cAMP pathway, for example, stimulates cellular gene expression by means of the PKA-mediated phosphorylation of cAMP-response element binding protein (CREB) at Ser-133. Here, we use genome-wide approaches to characterize target genes that are regulated by CREB in different cellular contexts. CREB was found to occupy approximately 4,000 promoter sites in vivo, depending on the presence and methylation state of consensus cAMP response elements near the promoter. The profiles for CREB occupancy were very similar in different human tissues, and exposure to a cAMP agonist stimulated CREB phosphorylation over a majority of these sites. Only a small proportion of CREB target genes was induced by cAMP in any cell type, however, due in part to the preferential recruitment of the coactivator CREB-binding protein to those promoters. These results indicate that CREB phosphorylation alone is not a reliable predictor of target gene activation and that additional CREB regulatory partners are required for recruitment of the transcriptional apparatus to the promoter.

SUBMITTER: Zhang X 

PROVIDER: S-EPMC555478 | biostudies-literature | 2005 Mar

REPOSITORIES: biostudies-literature

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Genome-wide analysis of cAMP-response element binding protein occupancy, phosphorylation, and target gene activation in human tissues.

Zhang Xinmin X   Odom Duncan T DT   Koo Seung-Hoi SH   Conkright Michael D MD   Canettieri Gianluca G   Best Jennifer J   Chen Huaming H   Jenner Richard R   Herbolsheimer Elizabeth E   Jacobsen Elizabeth E   Kadam Shilpa S   Ecker Joseph R JR   Emerson Beverly B   Hogenesch John B JB   Unterman Terry T   Young Richard A RA   Montminy Marc M  

Proceedings of the National Academy of Sciences of the United States of America 20050307 12


Hormones and nutrients often induce genetic programs via signaling pathways that interface with gene-specific activators. Activation of the cAMP pathway, for example, stimulates cellular gene expression by means of the PKA-mediated phosphorylation of cAMP-response element binding protein (CREB) at Ser-133. Here, we use genome-wide approaches to characterize target genes that are regulated by CREB in different cellular contexts. CREB was found to occupy approximately 4,000 promoter sites in vivo,  ...[more]

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