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Target-specific utilization of transcriptional regulatory surfaces by the glucocorticoid receptor.


ABSTRACT: The glucocorticoid receptor (GR) activates or represses transcription depending on the sequence and architecture of the glucocorticoid response elements in target genes and the availability and activity of interacting cofactors. Numerous GR cofactors have been identified, but they alone are insufficient to dictate the specificity of GR action. Furthermore, the role of different functional surfaces on the receptor itself in regulating its targets is unclear, due in part to the paucity of known target genes. Using DNA microarrays and real-time quantitative PCR, we identified genes transcriptionally activated by GR, in a translation-independent manner, in two human cell lines. We then assessed in U2OS osteosarcoma cells the consequences of individually disrupting three GR domains, the N-terminal activation function (AF) 1, the C-terminal AF2, or the dimer interface, on activation of these genes. We found that GR targets differed in their requirements for AF1 or AF2, and that the dimer interface was dispensable for activation of some genes in each class. Thus, in a single cell type, different GR surfaces were used in a gene-specific manner. These findings have strong implications for the nature of gene response element signaling, the composition and structure of regulatory complexes, and the mechanisms of context-specific transcriptional regulation.

SUBMITTER: Rogatsky I 

PROVIDER: S-EPMC283509 | biostudies-literature | 2003 Nov

REPOSITORIES: biostudies-literature

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Target-specific utilization of transcriptional regulatory surfaces by the glucocorticoid receptor.

Rogatsky Inez I   Wang Jen-Chywan JC   Derynck Mika K MK   Nonaka Daisuke F DF   Khodabakhsh Daniel B DB   Haqq Christopher M CM   Darimont Beatrice D BD   Garabedian Michael J MJ   Yamamoto Keith R KR  

Proceedings of the National Academy of Sciences of the United States of America 20031114 24


The glucocorticoid receptor (GR) activates or represses transcription depending on the sequence and architecture of the glucocorticoid response elements in target genes and the availability and activity of interacting cofactors. Numerous GR cofactors have been identified, but they alone are insufficient to dictate the specificity of GR action. Furthermore, the role of different functional surfaces on the receptor itself in regulating its targets is unclear, due in part to the paucity of known ta  ...[more]

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