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Molecular and Cellular Biology, March 2008, p. 1915-1923, Vol. 28, No. 6
0270-7306/08/$08.00+0 doi:10.1128/MCB.01541-07
Copyright © 2008, American Society for Microbiology. All Rights Reserved.
Doubling the Size of the Glucocorticoid Receptor Ligand Binding Pocket by Deacylcortivazol
Kelly Suino-Powell,1
Yong Xu,1
Chenghai Zhang,1
Yong-guang Tao,2
W. David Tolbert,1
S. Stoney Simons Jr.,2 and
H. Eric Xu1*
Laboratory of Structural Sciences, Van Andel Research Institute, 333 Bostwick Avenue, Grand Rapids, Michigan 49503,1 Steroid Hormones Section, NIDDK/CEB, National Institutes of Health, Bethesda, Maryland 20892-17722
Received 23 August 2007/ Returned for modification 10 October 2007/ Accepted 17 December 2007
A common feature of nuclear receptor ligand binding domains (LBD) is a helical sandwich fold that nests a ligand binding pocket within the bottom half of the domain. Here we report that the ligand pocket of glucocorticoid receptor (GR) can be continuously extended into the top half of the LBD by binding to deacylcortivazol (DAC), an extremely potent glucocorticoid. It has been puzzling for decades why DAC, which contains a phenylpyrazole replacement at the conserved 3-ketone of steroid hormones that are normally required for activation of their cognate receptors, is a potent GR activator. The crystal structure of the GR LBD bound to DAC and the fourth LXXLL motif of steroid receptor coactivator 1 reveals that the GR ligand binding pocket is expanded to a size of 1,070 Å3, effectively doubling the size of the GR dexamethasone-binding pocket of 540 Å3 and yet leaving the structure of the coactivator binding site intact. DAC occupies only 
50% of the space of the pocket but makes intricate interactions with the receptor around the phenylpyrazole group that accounts for the high-affinity binding of DAC. The dramatic expansion of the DAC-binding pocket thus highlights the conformational adaptability of GR to ligand binding. The new structure also allows docking of various nonsteroidal ligands that cannot be fitted into the previous structures, thus providing a new rational template for drug discovery of steroidal and nonsteroidal glucocorticoids that can be specifically designed to reach the unoccupied space of the expanded pocket.
* Corresponding author. Mailing address: Laboratory of Structural Sciences, Van Andel Research Institute, 333 Bostwick Avenue, Grand Rapids, MI 49503. Phone: (616) 234-5772. Fax: (616) 234-5773. E-mail: eric.xu{at}vai.org
Published ahead of print on 26 December 2007.
Molecular and Cellular Biology, March 2008, p. 1915-1923, Vol. 28, No. 6
0270-7306/08/$08.00+0 doi:10.1128/MCB.01541-07
Copyright © 2008, American Society for Microbiology. All Rights Reserved.
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