Literature DB >> 19574450

Inhibition of prostate cancer cell growth by second-site androgen receptor antagonists.

James D Joseph1, Bryan M Wittmann, Mary A Dwyer, Huaxia Cui, Delita A Dye, Donald P McDonnell, John D Norris.   

Abstract

The impact of ligand binding on nuclear receptor (NR) structure and the ability of target cells to distinguish between different receptor-ligand complexes are key determinants of the pharmacological activity of NR ligands. However, until relatively recently, these mechanistic insights have not been used in a prospective manner to develop screens for NR modulators with specific therapeutic activities. Driven by the need for unique androgen receptor (AR) antagonists that retain activity in hormone-refractory prostate cancer, we developed and applied a conformation-based screen to identify AR antagonists that were mechanistically distinct from existing drugs of this class. Two molecules were identified by using this approach, D36 and D80, which interact with AR in a unique manner and allosterically inhibit AR agonist activity. Unlike the clinically important antiandrogens, casodex and hydroxyflutamide, both D36 and D80 block androgen action in cellular models of hormone-refractory prostate cancer. Mechanistically, these compounds further distinguish themselves from classical AR antagonists in that they do not promote AR nuclear translocation and quantitatively inhibit the association of AR with DNA even under conditions of overexpression. Although the therapeutic potential of these antiandrogens is apparent, it is the demonstration that it is possible, to modulate the interaction of cofactors with agonist-activated AR, using second-site modulators, that has the greatest potential with respect to the therapeutic exploitation of AR and other NRs.

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Year:  2009        PMID: 19574450      PMCID: PMC2715477          DOI: 10.1073/pnas.0900185106

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  25 in total

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2.  Collocation of androgen receptor gene mutations in prostate cancer.

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4.  Progression of metastatic human prostate cancer to androgen independence in immunodeficient SCID mice.

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6.  Survey of gene amplifications during prostate cancer progression by high-throughout fluorescence in situ hybridization on tissue microarrays.

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7.  Molecular characterization of human prostate carcinoma cell lines.

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  16 in total

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Journal:  World J Urol       Date:  2011-08-11       Impact factor: 4.226

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Review 7.  Evolving landscape and novel treatments in metastatic castrate-resistant prostate cancer.

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Journal:  Asian J Androl       Date:  2013-04-15       Impact factor: 3.285

8.  Novel yeast-based strategy unveils antagonist binding regions on the nuclear xenobiotic receptor PXR.

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Review 9.  Minireview: Not picking pockets: nuclear receptor alternate-site modulators (NRAMs).

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Review 10.  Steroid Receptor-Associated Immunophilins: A Gateway to Steroid Signalling.

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