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This version published online on January 29, 2004
Molecular Endocrinology, doi:10.1210/me.2003-0157
Molecular Endocrinology Vol. 0, No. 2004 200301571-
doi:10.1210/me.2003-0157
Copyright © 2004 by the Endocrine Society.
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Submitted on April 24, 2003
Accepted on January 23, 2004

Steroid-Responsive Sequences in the Human Glucocorticoid Receptor Gene 1A Promoter

Chuan-dong Geng and Wayne V. Vedeckis*

Department of Biochemistry and Molecular Biology and Stanley S. Scott Cancer Center, Louisiana State University Health Sciences Center, New Orleans, Louisiana

* To whom correspondence should be addressed. E-mail: wvedec{at}lsuhsc.edu.

At least three promoters (1A, 1B, and 1C) control the expression of mRNA transcripts for the human glucocorticoid receptor (hGR) protein. An hGR 1A promoter/exon sequence (-218/+269) contains at least 12 DNase I footprints that contain bound protein. Whereas four of these footprints (FP6, FP7, FP8, and FP11) contain bound hGR in protein-DNA complexes that are formed, only two (FP7 and FP11) appear to be important for the up-regulation of hGR 1A promoter/exon activity in T-lymphoblasts. Furthermore, the activity of these DNA elements depends upon the promoter context, leading to a redundant and complex regulation of expression of the hGR 1A promoter/exon. FP7 appears to be required for hormonal responsiveness in the absence of upstream sequences (+41/+269), while the hormonal responsiveness of FP11 requires a functional, adjacent FP12 DNA sequence. FP12 contains overlapping binding sites for the protooncogene transcription factors c-Myb and c-Ets. It seems likely that binding of either c-Myb or c-Ets to FP12 is necessary for the direct or indirect binding of the hGR to FP11 (a non-consensus glucocorticoid response element), and the resultant steroid-responsiveness of the hGR 1A promoter/exon sequence. We propose that the identity of the accessory transcription factor bound to FP12 (c-Myb or c-Ets) may determine the nature of regulation (positive or negative) of hGR gene expression by hormone, and that this may be important for hormone-induced apoptosis in T-cell acute lymphoblastic leukemia.
Key words: glucocorticoid receptor • promoter 1A • up-regulation • ets • myb

NURSA Molecule Pages Link:

Nuclear Receptors:   GR
Ligands:   Dexamethasone



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