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dc.contributor.authorEskew, Jeffery D.
dc.contributor.authorSadikot, Takrima
dc.contributor.authorMorales, Pedro
dc.contributor.authorDuren, Alicia
dc.contributor.authorDunwiddie, Irene
dc.contributor.authorSwink, Megan
dc.contributor.authorZhang, Xiaoying
dc.contributor.authorHembruff, Stacey
dc.contributor.authorDonnelly, Alison
dc.contributor.authorRajewski, Roger A.
dc.contributor.authorBlagg, Brian S. J.
dc.contributor.authorManjarrez, Jacob R.
dc.contributor.authorMatts, Robert L.
dc.contributor.authorHolzbeierlein, Jeffrey M.
dc.contributor.authorVielhauer, George A.
dc.date.accessioned2018-11-09T21:10:43Z
dc.date.available2018-11-09T21:10:43Z
dc.date.issued2011-10-31
dc.identifieroksd_eskew_developmentandc_2011-10-31
dc.identifier.citationEskew, J. D., Sadikot, T., Morales, P., Duren, A., Dunwiddie, I., Swink, M. ... Vielhauer, G. A. (2011). Development and characterization of a novel C-terminal inhibitor of Hsp90 in androgen dependent and independent prostate cancer cells. BMC Cancer, 11, Article 468. https://doi.org/10.1186/1471-2407-11-468
dc.identifier.urihttps://hdl.handle.net/11244/302045
dc.description.abstractBackground: The molecular chaperone, heat shock protein 90 (Hsp90) has been shown to be overexpressed in a number of cancers, including prostate cancer, making it an important target for drug discovery. Unfortunately, results with N-terminal inhibitors from initial clinical trials have been disappointing, as toxicity and resistance resulting from induction of the heat shock response (HSR) has led to both scheduling and administration concerns. Therefore, Hsp90 inhibitors that do not induce the heat shock response represent a promising new direction for the treatment of prostate cancer. Herein, the development of a C-terminal Hsp90 inhibitor, KU174, is described, which demonstrates anti-cancer activity in prostate cancer cells in the absence of a HSR and describe a novel approach to characterize Hsp90 inhibition in cancer cells.
dc.description.abstractMethods: PC3-MM2 and LNCaP-LN3 cells were used in both direct and indirect in vitro Hsp90 inhibition assays (DARTS, Surface Plasmon Resonance, co-immunoprecipitation, luciferase, Western blot, anti-proliferative, cytotoxicity and size exclusion chromatography) to characterize the effects of KU174 in prostate cancer cells. Pilot in vivo efficacy studies were also conducted with KU174 in PC3-MM2 xenograft studies.
dc.description.abstractResults: KU174 exhibits robust anti-proliferative and cytotoxic activity along with client protein degradation and disruption of Hsp90 native complexes without induction of a HSR. Furthermore, KU174 demonstrates direct binding to the Hsp90 protein and Hsp90 complexes in cancer cells. In addition, in pilot in-vivo proof-of-concept studies KU174 demonstrates efficacy at 75 mg/kg in a PC3-MM2 rat tumor model.
dc.description.abstractConclusions: Overall, these findings suggest C-terminal Hsp90 inhibitors have potential as therapeutic agents for the treatment of prostate cancer.
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dc.languageen_US
dc.publisherBioMed Central
dc.rightsThis material has been previously published. In the Oklahoma State University Library's institutional repository this version is made available through the open access principles and the terms of agreement/consent between the author(s) and the publisher. The permission policy on the use, reproduction or distribution of the material falls under fair use for educational, scholarship, and research purposes. Contact Digital Resources and Discovery Services at lib-dls@okstate.edu or 405-744-9161 for further information.
dc.titleDevelopment and characterization of a novel C-terminal inhibitor of Hsp90 in androgen dependent and independent prostate cancer cells
osu.filenameoksd_eskew_developmentandc_2011-10-31.pdf
dc.description.peerreviewPeer reviewed
dc.identifier.doi10.1186/1471-2407-11-468
dc.description.departmentBiochemistry and Molecular Biology
dc.type.genreArticle
dc.type.materialText
dc.subject.keywordsHsp90
dc.subject.keywordsprostate cancer
dc.subject.keywordsnovobiocin
dc.subject.keywordsc-terminal inhibitors
dc.subject.keywordsn-terminal inhibitors


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