High-throughput screens identify HSP90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer

The development of new treatments for castrate resistant prostate cancer (CRPC) must address such challenges as intrinsic tumor heterogeneity and phenotypic plasticity. Combined PTEN/TP53 alterations represent a major genotype of CRPC (25–30%) and are associated with poor outcomes. Using tumor-deriv...

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Autores principales: Jansson, Keith H., Tucker, John B., Stahl, Lauren E., Simmons, John K., Fuller, Caitlyn, Beshiri, Michael L., Agarwal, Supreet, Fang, Lei, Hynes, Paul G., Alilin, Aian Neil, Lake, Ross, Abbey, Yasmine C., Cawley, Jacob, Tice, Caitlin M., Yin, JuanJuan, McKnight, Crystal, Klummp-Thomas, Carleen, Zhang, Xiaohu, Guha, Rajarshi, Hoover, Shelley, Simpson, R. Mark, Nguyen, Holly M., Corey, Eva, Thomas, Craig J., Proia, David A., Kelly, Kathleen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2018
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6250716/
https://www.ncbi.nlm.nih.gov/pubmed/30467317
http://dx.doi.org/10.1038/s41598-018-35417-0
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author Jansson, Keith H.
Tucker, John B.
Stahl, Lauren E.
Simmons, John K.
Fuller, Caitlyn
Beshiri, Michael L.
Agarwal, Supreet
Fang, Lei
Hynes, Paul G.
Alilin, Aian Neil
Lake, Ross
Abbey, Yasmine C.
Cawley, Jacob
Tice, Caitlin M.
Yin, JuanJuan
McKnight, Crystal
Klummp-Thomas, Carleen
Zhang, Xiaohu
Guha, Rajarshi
Hoover, Shelley
Simpson, R. Mark
Nguyen, Holly M.
Corey, Eva
Thomas, Craig J.
Proia, David A.
Kelly, Kathleen
author_facet Jansson, Keith H.
Tucker, John B.
Stahl, Lauren E.
Simmons, John K.
Fuller, Caitlyn
Beshiri, Michael L.
Agarwal, Supreet
Fang, Lei
Hynes, Paul G.
Alilin, Aian Neil
Lake, Ross
Abbey, Yasmine C.
Cawley, Jacob
Tice, Caitlin M.
Yin, JuanJuan
McKnight, Crystal
Klummp-Thomas, Carleen
Zhang, Xiaohu
Guha, Rajarshi
Hoover, Shelley
Simpson, R. Mark
Nguyen, Holly M.
Corey, Eva
Thomas, Craig J.
Proia, David A.
Kelly, Kathleen
author_sort Jansson, Keith H.
collection PubMed
description The development of new treatments for castrate resistant prostate cancer (CRPC) must address such challenges as intrinsic tumor heterogeneity and phenotypic plasticity. Combined PTEN/TP53 alterations represent a major genotype of CRPC (25–30%) and are associated with poor outcomes. Using tumor-derived, castration-resistant Pten/Tp53 null luminal prostate cells for comprehensive, high-throughput, mechanism-based screening, we identified several vulnerabilities among >1900 compounds, including inhibitors of: PI3K/AKT/mTOR, the proteasome, the cell cycle, heat shock proteins, DNA repair, NFκB, MAPK, and epigenetic modifiers. HSP90 inhibitors were one of the most active compound classes in the screen and have clinical potential for use in drug combinations to enhance efficacy and delay the development of resistance. To inform future design of rational drug combinations, we tested ganetespib, a potent second-generation HSP90 inhibitor, as a single agent in multiple CRPC genotypes and phenotypes. Ganetespib decreased growth of endogenous Pten/Tp53 null tumors, confirming therapeutic activity in situ. Fifteen human CRPC LuCaP PDX-derived organoid models were assayed for responses to 110 drugs, and HSP90 inhibitors (ganetespib and onalespib) were among the select group of drugs (<10%) that demonstrated broad activity (>75% of models) at high potency (IC50 <1 µM). Ganetespib inhibits multiple targets, including AR and PI3K pathways, which regulate mutually compensatory growth and survival signals in some forms of CRPC. Combined with castration, ganetespib displayed deeper PDX tumor regressions and delayed castration resistance relative to either monotherapy. In all, comprehensive data from near-patient models presents novel contexts for HSP90 inhibition in multiple CRPC genotypes and phenotypes, expands upon HSP90 inhibitors as simultaneous inhibitors of oncogenic signaling and resistance mechanisms, and suggests utility for combined HSP90/AR inhibition in CRPC.
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spelling pubmed-62507162018-11-29 High-throughput screens identify HSP90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer Jansson, Keith H. Tucker, John B. Stahl, Lauren E. Simmons, John K. Fuller, Caitlyn Beshiri, Michael L. Agarwal, Supreet Fang, Lei Hynes, Paul G. Alilin, Aian Neil Lake, Ross Abbey, Yasmine C. Cawley, Jacob Tice, Caitlin M. Yin, JuanJuan McKnight, Crystal Klummp-Thomas, Carleen Zhang, Xiaohu Guha, Rajarshi Hoover, Shelley Simpson, R. Mark Nguyen, Holly M. Corey, Eva Thomas, Craig J. Proia, David A. Kelly, Kathleen Sci Rep Article The development of new treatments for castrate resistant prostate cancer (CRPC) must address such challenges as intrinsic tumor heterogeneity and phenotypic plasticity. Combined PTEN/TP53 alterations represent a major genotype of CRPC (25–30%) and are associated with poor outcomes. Using tumor-derived, castration-resistant Pten/Tp53 null luminal prostate cells for comprehensive, high-throughput, mechanism-based screening, we identified several vulnerabilities among >1900 compounds, including inhibitors of: PI3K/AKT/mTOR, the proteasome, the cell cycle, heat shock proteins, DNA repair, NFκB, MAPK, and epigenetic modifiers. HSP90 inhibitors were one of the most active compound classes in the screen and have clinical potential for use in drug combinations to enhance efficacy and delay the development of resistance. To inform future design of rational drug combinations, we tested ganetespib, a potent second-generation HSP90 inhibitor, as a single agent in multiple CRPC genotypes and phenotypes. Ganetespib decreased growth of endogenous Pten/Tp53 null tumors, confirming therapeutic activity in situ. Fifteen human CRPC LuCaP PDX-derived organoid models were assayed for responses to 110 drugs, and HSP90 inhibitors (ganetespib and onalespib) were among the select group of drugs (<10%) that demonstrated broad activity (>75% of models) at high potency (IC50 <1 µM). Ganetespib inhibits multiple targets, including AR and PI3K pathways, which regulate mutually compensatory growth and survival signals in some forms of CRPC. Combined with castration, ganetespib displayed deeper PDX tumor regressions and delayed castration resistance relative to either monotherapy. In all, comprehensive data from near-patient models presents novel contexts for HSP90 inhibition in multiple CRPC genotypes and phenotypes, expands upon HSP90 inhibitors as simultaneous inhibitors of oncogenic signaling and resistance mechanisms, and suggests utility for combined HSP90/AR inhibition in CRPC. Nature Publishing Group UK 2018-11-22 /pmc/articles/PMC6250716/ /pubmed/30467317 http://dx.doi.org/10.1038/s41598-018-35417-0 Text en © The Author(s) 2018 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Jansson, Keith H.
Tucker, John B.
Stahl, Lauren E.
Simmons, John K.
Fuller, Caitlyn
Beshiri, Michael L.
Agarwal, Supreet
Fang, Lei
Hynes, Paul G.
Alilin, Aian Neil
Lake, Ross
Abbey, Yasmine C.
Cawley, Jacob
Tice, Caitlin M.
Yin, JuanJuan
McKnight, Crystal
Klummp-Thomas, Carleen
Zhang, Xiaohu
Guha, Rajarshi
Hoover, Shelley
Simpson, R. Mark
Nguyen, Holly M.
Corey, Eva
Thomas, Craig J.
Proia, David A.
Kelly, Kathleen
High-throughput screens identify HSP90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer
title High-throughput screens identify HSP90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer
title_full High-throughput screens identify HSP90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer
title_fullStr High-throughput screens identify HSP90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer
title_full_unstemmed High-throughput screens identify HSP90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer
title_short High-throughput screens identify HSP90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer
title_sort high-throughput screens identify hsp90 inhibitors as potent therapeutics that target inter-related growth and survival pathways in advanced prostate cancer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6250716/
https://www.ncbi.nlm.nih.gov/pubmed/30467317
http://dx.doi.org/10.1038/s41598-018-35417-0
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