Pituitary Ets-1 and GABP bind to the growth factor regulatory sites of the rat prolactin promoter

doi:10.1093/nar/29.5.1251

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Nucleic Acids Research, 2001, Vol. 29, No. 5 1251-1260
© 2001 Oxford University Press

Pituitary Ets-1 and GABP bind to the growth factor regulatory sites of the rat prolactin promoter

Rebecca E. Schweppe¹ and Arthur Gutierrez-Hartmann¹^,2^,*

¹Department of Biochemistry and Molecular Genetics and ²Department of Medicine, Program in Molecular Biology and Colorado Cancer Center, University of Colorado Health Sciences Center, 4200 East Ninth Avenue, Box B-151, Denver, CO 80262, USA

Ets factors play a critical role in oncogenic Ras- and growthfactor-mediated regulation of the proximal rat prolactin (rPRL)promoter in pituitary cells. The rPRL promoter contains twokey functional Ets binding sites (EBS): a composite EBS/Pit-1element located at –212 and an EBS that co-localizes withthe basal transcription element (BTE, or A-site) located at–96. Oncogenic Ras exclusively signals to the –212site, which we have named the Ras response element (RRE); whereasthe response of multiple growth factors (FGFs, EGF, IGF, insulinand TRH) maps to both EBSs. Although Ets-1 and GA binding protein(GABP) have been implicated in the Ras and insulin responses,respectively, the precise identity of the pituitary Ets factorsthat specifically bind to the RRE and BTE sites remains unknown.In order to identify the Ets factor(s) present in GH4 and GH3nuclear extracts (GH4NE and GH3NE) that bind to the EBSs containedin the RRE and BTE, we used EBS-RRE and BTE oligonucleotidesin electrophoretic mobility shift assays (EMSAs), antibody supershiftassays, western blot analysis of partially purified fractionsand UV-crosslinking studies. EMSAs, using either the BTE orEBS-RRE probes, identified a specific protein–DNA complex,designated complex A, which contains an Ets factor as determinedby oligonucleotide competition studies. Using western blot analysisof GH3 nuclear proteins that bind to heparin–Sepharose,we have shown that Ets-1 and GABP, which are MAP kinase substrates,co-purify with complex A, and supershift analysis with specificantisera revealed that complex A contains Ets-1, GABP ${alpha}$ and GABPß1.In addition, we show that recombinant full-length Ets-1 bindsequivalently to BTE and EBS-RRE probes, while recombinant GABP ${alpha}$ /ßpreferentially binds to the BTE probe. Furthermore, comparingthe DNA binding of GH4NE containing both Ets-1 and GABP andHeLa nuclear extracts devoid of Ets-1 but containing GABP, wewere able to show that the EBS-RRE preferentially binds Ets-1,while the BTE binds both GABP and Ets-1. Finally, UV-crosslinkingexperiments with radiolabeled EBS-RRE and BTE oligonucleotidesshowed that these probes specifically bind to a protein of $~$ 64 kDa,which is consistent with binding to Ets-1 (54 kDa) and/orthe DNA binding subunit of GABP, GABP ${alpha}$ (57 kDa). These studiesshow that endogenous, pituitary-derived GABP and Ets-1 bindto the BTE, whereas Ets-1 preferentially binds to the EBS-RRE.Taken together, these data provide important insights into themechanisms by which the combination of distinct Ets membersand EBSs transduce differential growth factor responses.

^* To whom correspondence should be addressed. Tel: +1 303 3158443; Fax: +1 303 315 4525; Email: a.gutierrez-hartmann{at}uchsc.edu

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