Johanny Tonos De Leon, Aki Iwai, Clementine Feau, Yenni Garcia, Heather A Balsiger, Cheryl L Storer, Raquel M Suro, Kristine M Garza, Sunmin Lee, Yeong Sang Kim, Yu Chen, Yang-Min Ning, Daniel L Riggs, Robert J Fletterick, R Kiplin Guy, Jane B Trepel, Leonard M Neckers, Marc B Cox
Index: Proc. Natl. Acad. Sci. U. S. A. 108(29) , 11878-83, (2011)
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Drugs that target novel surfaces on the androgen receptor (AR) and/or novel AR regulatory mechanisms are promising alternatives for the treatment of castrate-resistant prostate cancer. The 52 kDa FK506 binding protein (FKBP52) is an important positive regulator of AR in cellular and whole animal models and represents an attractive target for the treatment of prostate cancer. We used a modified receptor-mediated reporter assay in yeast to screen a diversified natural compound library for inhibitors of FKBP52-enhanced AR function. The lead compound, termed MJC13, inhibits AR function by preventing hormone-dependent dissociation of the Hsp90-FKBP52-AR complex, which results in less hormone-bound receptor in the nucleus. Assays in early and late stage human prostate cancer cells demonstrated that MJC13 inhibits AR-dependent gene expression and androgen-stimulated prostate cancer cell proliferation.
Structure | Name/CAS No. | Molecular Formula | Articles |
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N-(2,3-dichlorophenyl)cyclohexanecarboxamide
CAS:200709-97-3 |
C13H15Cl2NO |
Similarities and Distinctions in Actions of Surface-Directed...
2015-01-01 [PLoS ONE 10(9) , e0137103, (2015)] |
The FKBP52 Cochaperone Acts in Synergy with β-Catenin to Pot...
2015-01-01 [PLoS ONE 10(7) , e0134015, (2015)] |
Quantification of a New Anti-Cancer Molecule MJC13 Using a R...
2015-01-01 [Am. J. Mod. Chromatogr. 1(1) , 1-11, (2014)] |
Androgen receptor splice variants are resistant to inhibitor...
2013-06-01 [Steroids 78(6) , 548-54, (2013)] |
Solution formulation development and efficacy of MJC13 in a ...
2016-01-01 [Pharm. Dev. Technol. 21(1) , 121-6, (2016)] |
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