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0013-722714572004JulEndocrinologyEndocrinologyConcerted regulation of the porcine steroidogenic acute regulatory protein gene promoter activity by follicle-stimulating hormone and insulin-like growth factor I in granulosa cells involves GATA-4 and CCAAT/enhancer binding protein beta.312231343122-34We previously demonstrated that FSH alone or in combination with IGF-I activated the porcine steroidogenic acute regulatory protein gene promoter in a concerted manner in primary cultures of granulosa cells. Studies were undertaken to further delineate cis- and trans-acting elements of the porcine promoter and mechanisms mediating FSH stimulation and its augmentation by IGF-I. Mutation of several putative regulatory elements localized hormone-stimulated activity to the highly conserved GATA site and identified novel nucleotides downstream as a functional CCAAT/enhancer binding protein (C/EBP)beta site. In granulosa cell nuclear extracts, GATA-4 and C/EBPbeta formed a high-molecular-weight complex with an oligonucleotide spanning -76 to -32 bp of the porcine promoter. The intensity of this high-molecular-weight complex was increased in granulosa cell nuclear extracts by treatment with FSH alone and was enhanced with the combination of FSH and IGF-I at 2-3 h of treatment. GATA-4 and C/EBPbeta proteins were uniformly expressed with all treatments at time points associated with increased DNA binding. Treatment (2 h) with FSH alone or FSH + IGF-I increased phosphorylation of GATA-4 on a protein kinase A consensus site. The 38-kDa isoform of C/EBPbeta exhibited greater phosphorylation with FSH + IGF-I treatment. Porcine luteal cell nuclear extracts also demonstrated GATA-4 and C/EBPbeta binding to the -76 to -32 bp region of the promoter providing evidence for their cooperation in vivo. These data indicate that GATA-4 and C/EBPbeta are both required for FSH +/- IGF-I stimulation of the porcine steroidogenic acute regulatory protein gene promoter in homologous granulosa cell cultures.LaVoieHolly AHADepartment of Cell and Developmental Biology and Anatomy, Building 1, University of South Carolina School of Medicine, Columbia, South Carolina 29208, USA. hlavoie@med.sc.edu.SinghDheerDHuiYvonne YYYengHD-038945HDNICHD NIH HHSUnited StatesJournal ArticleResearch Support, Non-U.S. Gov'tResearch Support, U.S. Gov't, P.H.S.20040401
United StatesEndocrinology03750400013-72270CCAAT-Enhancer-Binding Protein-beta0DNA-Binding Proteins0GATA4 Transcription Factor0Phosphoproteins0Transcription Factors0Steroidogenic Acute Regulatory Protein67763-96-6Insulin-Like Growth Factor I9002-68-0Follicle Stimulating HormoneIMAnimalsBase SequenceCCAAT-Enhancer-Binding Protein-betametabolismCells, CulturedDNA-Binding ProteinsmetabolismFemaleFollicle Stimulating HormonepharmacologyGATA4 Transcription FactorGranulosa Cellscytologydrug effectsphysiologyInsulin-Like Growth Factor IpharmacologyMolecular Sequence DataMutagenesis, Site-DirectedPhosphoproteinsgeneticsPhosphorylationPromoter Regions, GeneticphysiologySus scrofaTranscription FactorsmetabolismTransfectionSteroidogenic Acute Regulatory Protein2004435020047155020044350ppublish1505995110.1210/en.2003-1719en.2003-1719