Differential regulation of gene expression by insulin and IGF-1 receptors correlates with phosphorylation of a single amino acid residue in the forkhead transcription factor FKHR

Differential regulation of gene expression by insulin and IGF-1 receptors correlates with phosphorylation of a single amino acid residue in the forkhead transcription factor FKHR

The transcription factor FKHR is inhibited by phosphorylation in response to insulin and IGF‐1 through Akt kinase. Here we show that FKHR phosphorylation in hepatocytes conforms to a hierarchical pattern in which phosphorylation of the Akt site at S253, in the forkhead DNA binding domain, is a prere...

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Bibliographic Details
Published in:The EMBO journal Vol. 19; no. 5; pp. 989 - 996
Main Authors: Nakae, Jun, Barr, Valarie, Accili, Domenico
Format: Journal Article
Language:English
Published: Chichester, UK John Wiley & Sons, Ltd 01-03-2000
Blackwell Publishing Ltd
Oxford University Press
Subjects:
Akt kinase
Amino acids
Animals
Cell Line, Transformed
DNA-Binding Proteins - genetics
DNA-Binding Proteins - metabolism
FKHR protein
Forkhead Box Protein O1
forkhead protein
Forkhead Transcription Factors
gene expression
Gene Expression Regulation - drug effects
hepatocyte
Hypoglycemic Agents - metabolism
Hypoglycemic Agents - pharmacology
insulin
Insulin - metabolism
Insulin - pharmacology
insulin receptors
Insulin-Like Growth Factor I - metabolism
Insulin-Like Growth Factor I - pharmacology
kinase
Liver
Mice
Phosphorylation
Receptor, IGF Type 1 - genetics
Receptor, IGF Type 1 - metabolism
Receptor, Insulin - genetics
Receptor, Insulin - metabolism
Signal Transduction - drug effects
Transcription Factors - genetics
Transcription Factors - metabolism
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Summary:The transcription factor FKHR is inhibited by phosphorylation in response to insulin and IGF‐1 through Akt kinase. Here we show that FKHR phosphorylation in hepatocytes conforms to a hierarchical pattern in which phosphorylation of the Akt site at S253, in the forkhead DNA binding domain, is a prerequisite for the phosphorylation of two additional potential Akt sites, T24 and S316. Using insulin receptor‐deficient hepatocytes, we show that T24 fails to be phosphorylated by IGF‐1 receptors, suggesting that this residue is targeted by a kinase specifically activated by insulin receptors. Lack of T24 phosphorylation is associated with the failure of IGF‐1 to induce nuclear export of FKHR, and to inhibit expression of a reporter gene under the transcriptional control of the IGF binding protein‐1 insulin response element. We propose that site‐specific phosphorylation of FKHR is one of the mechanisms by which insulin and IGF‐1 receptors exert different effects on gene expression.
Bibliography:ArticleID:EMBJ7592211
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ark:/67375/WNG-TVGGHFJT-B
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SourceType-Scholarly Journals-1
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Corresponding author e-mail: da230@columbia.edu
ISSN:0261-4189
1460-2075
DOI:10.1093/emboj/19.5.989