Inhibition of the Human Hsc70 System by Small Ligands as a Potential Anticancer Approach

SIMPLE SUMMARY: High levels of Heat shock proteins (Hsps) in specific cancers are usually linked to a poor prognosis, tumor progression, invasiveness, and resistance to treatment. Chaperone inhibition could therefore be toxic for cancer cells due to their high dependence on chaperone activity to sur...

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Autores principales: Dublang, Leire, Underhaug, Jarl, Flydal, Marte I., Velasco-Carneros, Lorea, Maréchal, Jean-Didier, Moro, Fernando, Boyano, Maria Dolores, Martinez, Aurora, Muga, Arturo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8230956/
https://www.ncbi.nlm.nih.gov/pubmed/34208232
http://dx.doi.org/10.3390/cancers13122936
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author Dublang, Leire
Underhaug, Jarl
Flydal, Marte I.
Velasco-Carneros, Lorea
Maréchal, Jean-Didier
Moro, Fernando
Boyano, Maria Dolores
Martinez, Aurora
Muga, Arturo
author_facet Dublang, Leire
Underhaug, Jarl
Flydal, Marte I.
Velasco-Carneros, Lorea
Maréchal, Jean-Didier
Moro, Fernando
Boyano, Maria Dolores
Martinez, Aurora
Muga, Arturo
author_sort Dublang, Leire
collection PubMed
description SIMPLE SUMMARY: High levels of Heat shock proteins (Hsps) in specific cancers are usually linked to a poor prognosis, tumor progression, invasiveness, and resistance to treatment. Chaperone inhibition could therefore be toxic for cancer cells due to their high dependence on chaperone activity to survive. This study shows the potential to repurpose the small chemical compound pinaverium bromide, currently used to treat functional gastrointestinal disorders, as a possible antitumor drug since it displays a marked toxicity against two melanoma cell lines without affecting the viability of fibroblast and primary melanocytes. This compound interacts with structural regions shared by representatives of the Hsp70 and Hsp110 families, inhibiting the substrate remodeling ability of the Hsp70 system in vitro and in a cellular context. ABSTRACT: Heat shock protein (Hsp) synthesis is upregulated in a wide range of cancers to provide the appropriate environment for tumor progression. The Hsp110 and Hsp70 families have been associated to cancer cell survival and resistance to chemotherapy. In this study, we explore the strategy of drug repurposing to find new Hsp70 and Hsp110 inhibitors that display toxicity against melanoma cancer cells. We found that the hits discovered using Apg2, a human representative of the Hsp110 family, as the initial target bind also to structural regions present in members of the Hsp70 family, and therefore inhibit the remodeling activity of the Hsp70 system. One of these compounds, the spasmolytic agent pinaverium bromide used for functional gastrointestinal disorders, inhibits the intracellular chaperone activity of the Hsp70 system and elicits its cytotoxic activity specifically in two melanoma cell lines by activating apoptosis. Docking and molecular dynamics simulations indicate that this compound interacts with regions located in the nucleotide-binding domain and the linker of the chaperones, modulating their ATPase activity. Thus, repurposing of pinaverium bromide for cancer treatment appears as a promising novel therapeutic approach.
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spelling pubmed-82309562021-06-26 Inhibition of the Human Hsc70 System by Small Ligands as a Potential Anticancer Approach Dublang, Leire Underhaug, Jarl Flydal, Marte I. Velasco-Carneros, Lorea Maréchal, Jean-Didier Moro, Fernando Boyano, Maria Dolores Martinez, Aurora Muga, Arturo Cancers (Basel) Article SIMPLE SUMMARY: High levels of Heat shock proteins (Hsps) in specific cancers are usually linked to a poor prognosis, tumor progression, invasiveness, and resistance to treatment. Chaperone inhibition could therefore be toxic for cancer cells due to their high dependence on chaperone activity to survive. This study shows the potential to repurpose the small chemical compound pinaverium bromide, currently used to treat functional gastrointestinal disorders, as a possible antitumor drug since it displays a marked toxicity against two melanoma cell lines without affecting the viability of fibroblast and primary melanocytes. This compound interacts with structural regions shared by representatives of the Hsp70 and Hsp110 families, inhibiting the substrate remodeling ability of the Hsp70 system in vitro and in a cellular context. ABSTRACT: Heat shock protein (Hsp) synthesis is upregulated in a wide range of cancers to provide the appropriate environment for tumor progression. The Hsp110 and Hsp70 families have been associated to cancer cell survival and resistance to chemotherapy. In this study, we explore the strategy of drug repurposing to find new Hsp70 and Hsp110 inhibitors that display toxicity against melanoma cancer cells. We found that the hits discovered using Apg2, a human representative of the Hsp110 family, as the initial target bind also to structural regions present in members of the Hsp70 family, and therefore inhibit the remodeling activity of the Hsp70 system. One of these compounds, the spasmolytic agent pinaverium bromide used for functional gastrointestinal disorders, inhibits the intracellular chaperone activity of the Hsp70 system and elicits its cytotoxic activity specifically in two melanoma cell lines by activating apoptosis. Docking and molecular dynamics simulations indicate that this compound interacts with regions located in the nucleotide-binding domain and the linker of the chaperones, modulating their ATPase activity. Thus, repurposing of pinaverium bromide for cancer treatment appears as a promising novel therapeutic approach. MDPI 2021-06-11 /pmc/articles/PMC8230956/ /pubmed/34208232 http://dx.doi.org/10.3390/cancers13122936 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Dublang, Leire
Underhaug, Jarl
Flydal, Marte I.
Velasco-Carneros, Lorea
Maréchal, Jean-Didier
Moro, Fernando
Boyano, Maria Dolores
Martinez, Aurora
Muga, Arturo
Inhibition of the Human Hsc70 System by Small Ligands as a Potential Anticancer Approach
title Inhibition of the Human Hsc70 System by Small Ligands as a Potential Anticancer Approach
title_full Inhibition of the Human Hsc70 System by Small Ligands as a Potential Anticancer Approach
title_fullStr Inhibition of the Human Hsc70 System by Small Ligands as a Potential Anticancer Approach
title_full_unstemmed Inhibition of the Human Hsc70 System by Small Ligands as a Potential Anticancer Approach
title_short Inhibition of the Human Hsc70 System by Small Ligands as a Potential Anticancer Approach
title_sort inhibition of the human hsc70 system by small ligands as a potential anticancer approach
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8230956/
https://www.ncbi.nlm.nih.gov/pubmed/34208232
http://dx.doi.org/10.3390/cancers13122936
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