Etoposide-Induced Apoptosis in Cancer Cells Can Be Reinforced by an Uncoupled Link between Hsp70 and Caspase-3

The Hsp70 chaperone binds and inhibits proteins implicated in apoptotic signaling including Caspase-3. Induction of apoptosis is an important mechanism of anti-cancer drugs, therefore Hsp70 can act as a protective system in tumor cells against therapeutic agents. In this study we present an assessme...

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Autores principales: Sverchinsky, Dmitry V., Nikotina, Alina D., Komarova, Elena Y., Mikhaylova, Elena R., Aksenov, Nikolay D., Lazarev, Vladimir F., Mitkevich, Vladimir A., Suezov, Roman, Druzhilovskiy, Dmitry S., Poroikov, Vladimir V., Margulis, Boris A., Guzhova, Irina V.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2018
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6163214/
https://www.ncbi.nlm.nih.gov/pubmed/30149619
http://dx.doi.org/10.3390/ijms19092519
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author Sverchinsky, Dmitry V.
Nikotina, Alina D.
Komarova, Elena Y.
Mikhaylova, Elena R.
Aksenov, Nikolay D.
Lazarev, Vladimir F.
Mitkevich, Vladimir A.
Suezov, Roman
Druzhilovskiy, Dmitry S.
Poroikov, Vladimir V.
Margulis, Boris A.
Guzhova, Irina V.
author_facet Sverchinsky, Dmitry V.
Nikotina, Alina D.
Komarova, Elena Y.
Mikhaylova, Elena R.
Aksenov, Nikolay D.
Lazarev, Vladimir F.
Mitkevich, Vladimir A.
Suezov, Roman
Druzhilovskiy, Dmitry S.
Poroikov, Vladimir V.
Margulis, Boris A.
Guzhova, Irina V.
author_sort Sverchinsky, Dmitry V.
collection PubMed
description The Hsp70 chaperone binds and inhibits proteins implicated in apoptotic signaling including Caspase-3. Induction of apoptosis is an important mechanism of anti-cancer drugs, therefore Hsp70 can act as a protective system in tumor cells against therapeutic agents. In this study we present an assessment of candidate compounds that are able to dissociate the complex of Hsp70 with Caspase-3, and thus sensitize cells to drug-induced apoptosis. Using the PASS program for prediction of biological activity we selected a derivative of benzodioxol (BT44) that is known to affect molecular chaperones and caspases. Drug affinity responsive target stability and microscale thermophoresis assays indicated that BT44 bound to Hsp70 and reduced the chaperone activity. When etoposide was administered, heat shock accompanied with an accumulation of Hsp70 led to an inhibition of etoposide-induced apoptosis. The number of apoptotic cells increased following BT44 administration, and forced Caspase-3 processing. Competitive protein–protein interaction and immunoprecipitation assays showed that BT44 caused dissociation of the Hsp70–Caspase-3 complex, thus augmenting the anti-tumor activity of etoposide and highlighting the potential role of molecular separators in cancer therapy.
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spelling pubmed-61632142018-10-10 Etoposide-Induced Apoptosis in Cancer Cells Can Be Reinforced by an Uncoupled Link between Hsp70 and Caspase-3 Sverchinsky, Dmitry V. Nikotina, Alina D. Komarova, Elena Y. Mikhaylova, Elena R. Aksenov, Nikolay D. Lazarev, Vladimir F. Mitkevich, Vladimir A. Suezov, Roman Druzhilovskiy, Dmitry S. Poroikov, Vladimir V. Margulis, Boris A. Guzhova, Irina V. Int J Mol Sci Article The Hsp70 chaperone binds and inhibits proteins implicated in apoptotic signaling including Caspase-3. Induction of apoptosis is an important mechanism of anti-cancer drugs, therefore Hsp70 can act as a protective system in tumor cells against therapeutic agents. In this study we present an assessment of candidate compounds that are able to dissociate the complex of Hsp70 with Caspase-3, and thus sensitize cells to drug-induced apoptosis. Using the PASS program for prediction of biological activity we selected a derivative of benzodioxol (BT44) that is known to affect molecular chaperones and caspases. Drug affinity responsive target stability and microscale thermophoresis assays indicated that BT44 bound to Hsp70 and reduced the chaperone activity. When etoposide was administered, heat shock accompanied with an accumulation of Hsp70 led to an inhibition of etoposide-induced apoptosis. The number of apoptotic cells increased following BT44 administration, and forced Caspase-3 processing. Competitive protein–protein interaction and immunoprecipitation assays showed that BT44 caused dissociation of the Hsp70–Caspase-3 complex, thus augmenting the anti-tumor activity of etoposide and highlighting the potential role of molecular separators in cancer therapy. MDPI 2018-08-25 /pmc/articles/PMC6163214/ /pubmed/30149619 http://dx.doi.org/10.3390/ijms19092519 Text en © 2018 by the authors. 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 (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Sverchinsky, Dmitry V.
Nikotina, Alina D.
Komarova, Elena Y.
Mikhaylova, Elena R.
Aksenov, Nikolay D.
Lazarev, Vladimir F.
Mitkevich, Vladimir A.
Suezov, Roman
Druzhilovskiy, Dmitry S.
Poroikov, Vladimir V.
Margulis, Boris A.
Guzhova, Irina V.
Etoposide-Induced Apoptosis in Cancer Cells Can Be Reinforced by an Uncoupled Link between Hsp70 and Caspase-3
title Etoposide-Induced Apoptosis in Cancer Cells Can Be Reinforced by an Uncoupled Link between Hsp70 and Caspase-3
title_full Etoposide-Induced Apoptosis in Cancer Cells Can Be Reinforced by an Uncoupled Link between Hsp70 and Caspase-3
title_fullStr Etoposide-Induced Apoptosis in Cancer Cells Can Be Reinforced by an Uncoupled Link between Hsp70 and Caspase-3
title_full_unstemmed Etoposide-Induced Apoptosis in Cancer Cells Can Be Reinforced by an Uncoupled Link between Hsp70 and Caspase-3
title_short Etoposide-Induced Apoptosis in Cancer Cells Can Be Reinforced by an Uncoupled Link between Hsp70 and Caspase-3
title_sort etoposide-induced apoptosis in cancer cells can be reinforced by an uncoupled link between hsp70 and caspase-3
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6163214/
https://www.ncbi.nlm.nih.gov/pubmed/30149619
http://dx.doi.org/10.3390/ijms19092519
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