Dual targeting of HSP70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer

Muscle invasive bladder cancer (MIBC) is a common malignancy and major cause of morbidity worldwide. Over the last decade mortality rates for MIBC have not decreased as compared to other cancers indicating a need for novel strategies. The molecular chaperones HSP70 and HSP90 fold and maintain the 3-...

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Autores principales: Prince, Thomas, Ackerman, Andrew, Cavanaugh, Alice, Schreiter, Brielle, Juengst, Brendon, Andolino, Chaylen, Danella, John, Chernin, Mitch, Williams, Heinric
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6135696/
https://www.ncbi.nlm.nih.gov/pubmed/30220976
http://dx.doi.org/10.18632/oncotarget.26021
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author Prince, Thomas
Ackerman, Andrew
Cavanaugh, Alice
Schreiter, Brielle
Juengst, Brendon
Andolino, Chaylen
Danella, John
Chernin, Mitch
Williams, Heinric
author_facet Prince, Thomas
Ackerman, Andrew
Cavanaugh, Alice
Schreiter, Brielle
Juengst, Brendon
Andolino, Chaylen
Danella, John
Chernin, Mitch
Williams, Heinric
author_sort Prince, Thomas
collection PubMed
description Muscle invasive bladder cancer (MIBC) is a common malignancy and major cause of morbidity worldwide. Over the last decade mortality rates for MIBC have not decreased as compared to other cancers indicating a need for novel strategies. The molecular chaperones HSP70 and HSP90 fold and maintain the 3-dimensional structures of numerous client proteins that signal for cancer cell growth and survival. Inhibition of HSP70 or HSP90 results in client protein degradation and associated oncogenic signaling. Here we targeted HSP70 and HSP90 with small molecule inhibitors that trap or block each chaperone in a low client-affinity “open” conformation. HSP70 inhibitors, VER155008 (VER) and MAL3-101 (MAL), along with HSP90 inhibitor, STA-9090 (STA), were tested alone and in combination for their ability to reduce cell viability and alter protein levels in 4 MIBC cell lines. When combined, VER+MAL synergistically reduced cell viability in each MIBC cell line while not inducing expression of heat shock proteins (HSPs). STA+MAL also synergistically reduced cell viability in each cell line but induced expression of cytoprotective HSPs indicating the merits of targeting HSP70 with VER+MAL. Additionally, we observed that STA induced the expression of the stress-related transcription factor HSF2 while reducing levels of the co-chaperone TTI1.
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spelling pubmed-61356962018-09-14 Dual targeting of HSP70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer Prince, Thomas Ackerman, Andrew Cavanaugh, Alice Schreiter, Brielle Juengst, Brendon Andolino, Chaylen Danella, John Chernin, Mitch Williams, Heinric Oncotarget Research Paper Muscle invasive bladder cancer (MIBC) is a common malignancy and major cause of morbidity worldwide. Over the last decade mortality rates for MIBC have not decreased as compared to other cancers indicating a need for novel strategies. The molecular chaperones HSP70 and HSP90 fold and maintain the 3-dimensional structures of numerous client proteins that signal for cancer cell growth and survival. Inhibition of HSP70 or HSP90 results in client protein degradation and associated oncogenic signaling. Here we targeted HSP70 and HSP90 with small molecule inhibitors that trap or block each chaperone in a low client-affinity “open” conformation. HSP70 inhibitors, VER155008 (VER) and MAL3-101 (MAL), along with HSP90 inhibitor, STA-9090 (STA), were tested alone and in combination for their ability to reduce cell viability and alter protein levels in 4 MIBC cell lines. When combined, VER+MAL synergistically reduced cell viability in each MIBC cell line while not inducing expression of heat shock proteins (HSPs). STA+MAL also synergistically reduced cell viability in each cell line but induced expression of cytoprotective HSPs indicating the merits of targeting HSP70 with VER+MAL. Additionally, we observed that STA induced the expression of the stress-related transcription factor HSF2 while reducing levels of the co-chaperone TTI1. Impact Journals LLC 2018-08-24 /pmc/articles/PMC6135696/ /pubmed/30220976 http://dx.doi.org/10.18632/oncotarget.26021 Text en Copyright: © 2018 Prince et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License 3.0 (http://creativecommons.org/licenses/by/3.0/) (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Prince, Thomas
Ackerman, Andrew
Cavanaugh, Alice
Schreiter, Brielle
Juengst, Brendon
Andolino, Chaylen
Danella, John
Chernin, Mitch
Williams, Heinric
Dual targeting of HSP70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer
title Dual targeting of HSP70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer
title_full Dual targeting of HSP70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer
title_fullStr Dual targeting of HSP70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer
title_full_unstemmed Dual targeting of HSP70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer
title_short Dual targeting of HSP70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer
title_sort dual targeting of hsp70 does not induce the heat shock response and synergistically reduces cell viability in muscle invasive bladder cancer
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6135696/
https://www.ncbi.nlm.nih.gov/pubmed/30220976
http://dx.doi.org/10.18632/oncotarget.26021
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