AI Article Synopsis

  • SF-1, an orphan nuclear receptor in the adrenal cortex and gonads, regulates genes involved in steroid hormone production through hormonal stimulation.
  • SUMOylation of SF-1 at K194 does not change its location within the cell, but it inhibits its ability to activate target genes, while loss of this modification enhances SF-1 phosphorylation at serine 203.
  • The study suggests a model where SUMOylation reduces SF-1's transcriptional activity in adrenocortical cancer cells by limiting CDK7-induced phosphorylation, affecting the expression of steroidogenic enzyme genes.

Article Abstract

Steroidogenic factor 1 (SF-1) is an orphan nuclear receptor selectively expressed in the adrenal cortex and gonads, where it mediates the hormonal stimulation of multiple genes involved in steroid hormone biosynthesis. SF-1 is the target of both phosphorylation and SUMOylation, but how these modifications interact or contribute to SF-1 regulation of endogenous genes remains poorly defined. We found that SF-1 is selectively SUMOylated at K194 in Y1 adrenocarcinoma cells and that although SUMOylation does not alter the subcellular localization of SF-1, the modification inhibits the ability of SF-1 to activate target genes. Notably, whereas SF-1 SUMOylation is independent of S203 phosphorylation and is unaffected by adrenocorticotropin (ACTH) treatment, loss of SUMOylation leads to enhanced SF-1 phosphorylation at serine 203. Furthermore, preventing SF-1 SUMOylation increases the mRNA and protein levels of multiple steroidogenic enzyme genes. Analysis of the StAR promoter indicates that blockade of SF-1 SUMOylation leads to an increase in overall promoter occupancy but does not alter the oscillatory recruitment dynamics in response to ACTH. Notably, we find that CDK7 binds preferentially to the SUMOylation-deficient form of SF-1 and that CDK7 inhibition reduces phosphorylation of SF-1. Based on these observations, we propose a coordinated modification model in which inhibition of SF-1-mediated transcription by SUMOylation in adrenocortical cancer cells is mediated through reduced CDK7-induced phosphorylation of SF-1.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2630698PMC
http://dx.doi.org/10.1128/MCB.00295-08DOI Listing

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