Cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells

Etoposide (ETP) and anthracyclines are applied for wide anti-cancer treatments. However, the ETP-induced cardiotoxicity remains to be a major safety issue and the underlying cardiotoxic mechanisms are not well understood. This study is aiming to unravel the cardiotoxicity profile of ETP in compariso...

Descripción completa

Detalles Bibliográficos
Autores principales: Nemade, Harshal, Chaudhari, Umesh, Acharya, Aviseka, Hescheler, Jürgen, Hengstler, Jan Georg, Papadopoulos, Symeon, Sachinidis, Agapios
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Berlin Heidelberg 2018
Materias:
In Vitro Systems
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5882643/
https://www.ncbi.nlm.nih.gov/pubmed/29397400
http://dx.doi.org/10.1007/s00204-018-2170-7
_version_ 1783311488133365760
author Nemade, Harshal
Chaudhari, Umesh
Acharya, Aviseka
Hescheler, Jürgen
Hengstler, Jan Georg
Papadopoulos, Symeon
Sachinidis, Agapios
author_facet Nemade, Harshal
Chaudhari, Umesh
Acharya, Aviseka
Hescheler, Jürgen
Hengstler, Jan Georg
Papadopoulos, Symeon
Sachinidis, Agapios
author_sort Nemade, Harshal
collection PubMed
description Etoposide (ETP) and anthracyclines are applied for wide anti-cancer treatments. However, the ETP-induced cardiotoxicity remains to be a major safety issue and the underlying cardiotoxic mechanisms are not well understood. This study is aiming to unravel the cardiotoxicity profile of ETP in comparison to anthracyclines using physiologically relevant human pluripotent stem cell-derived cardiomyocytes (hPSC-CMs). Using xCELLigence real-time cell analyser (RTCA), we found that single high dose of ETP induces irreversible increase in hPSC-CMs beating rate and decrease in beating amplitude. We also identified 58 deregulated genes consisting of 33 upregulated and 25 downregulated genes in hPSC-CMs after ETP treatment. Gene ontology (GO) and pathway analysis showed that most upregulated genes are enriched in GO categories like positive regulation of apoptotic process, regulation of cell death, and mitochondria organization, whereas most downregulated genes were enriched in GO categories like cytoskeletal organization, muscle contraction, and Ca(2+) ion homeostasis. Moreover, we also found upregulation in 5 miRNAs (has-miR-486-3p, has-miR-34c-5p, has-miR-4423-3p, has-miR-182-5p, and has-miR-139-5p) which play role in muscle contraction, arginine and proline metabolism, and hypertrophic cardiomyopathy (HCM). Immunostaining and transmission electron microscopy also confirmed the cytoskeletal and mitochondrial damage in hPSC-CMs treated with ETP, as well as noticeable alterations in intracellular calcium handling and mitochondrial membrane potential were also observed. The apoptosis inhibitor, Pifithrin-α, found to protect hPSC-CMs from ETP-induced cardiotoxicity, whereas hPSC-CMs treated with ferroptosis inhibitor, Liproxstatin-1, showed significant recovery in hPSC-CMs functional properties like beating rate and amplitude after ETP treatment. We suggest that the damage to mitochondria is a major contributing factor involved in ETP-induced cardiotoxicity and the activation of the p53-mediated ferroptosis pathway by ETP is likely the critical pathway in ETP-induced cardiotoxicity. We also conclude that the genomic biomarkers identified in this study will significantly contribute to develop and predict potential cardiotoxic effects of novel anti-cancer drugs in vitro. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00204-018-2170-7) contains supplementary material, which is available to authorized users.
format Online
Article
Text
id pubmed-5882643
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Springer Berlin Heidelberg
record_format MEDLINE/PubMed
spelling pubmed-58826432018-04-05 Cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells Nemade, Harshal Chaudhari, Umesh Acharya, Aviseka Hescheler, Jürgen Hengstler, Jan Georg Papadopoulos, Symeon Sachinidis, Agapios Arch Toxicol In Vitro Systems Etoposide (ETP) and anthracyclines are applied for wide anti-cancer treatments. However, the ETP-induced cardiotoxicity remains to be a major safety issue and the underlying cardiotoxic mechanisms are not well understood. This study is aiming to unravel the cardiotoxicity profile of ETP in comparison to anthracyclines using physiologically relevant human pluripotent stem cell-derived cardiomyocytes (hPSC-CMs). Using xCELLigence real-time cell analyser (RTCA), we found that single high dose of ETP induces irreversible increase in hPSC-CMs beating rate and decrease in beating amplitude. We also identified 58 deregulated genes consisting of 33 upregulated and 25 downregulated genes in hPSC-CMs after ETP treatment. Gene ontology (GO) and pathway analysis showed that most upregulated genes are enriched in GO categories like positive regulation of apoptotic process, regulation of cell death, and mitochondria organization, whereas most downregulated genes were enriched in GO categories like cytoskeletal organization, muscle contraction, and Ca(2+) ion homeostasis. Moreover, we also found upregulation in 5 miRNAs (has-miR-486-3p, has-miR-34c-5p, has-miR-4423-3p, has-miR-182-5p, and has-miR-139-5p) which play role in muscle contraction, arginine and proline metabolism, and hypertrophic cardiomyopathy (HCM). Immunostaining and transmission electron microscopy also confirmed the cytoskeletal and mitochondrial damage in hPSC-CMs treated with ETP, as well as noticeable alterations in intracellular calcium handling and mitochondrial membrane potential were also observed. The apoptosis inhibitor, Pifithrin-α, found to protect hPSC-CMs from ETP-induced cardiotoxicity, whereas hPSC-CMs treated with ferroptosis inhibitor, Liproxstatin-1, showed significant recovery in hPSC-CMs functional properties like beating rate and amplitude after ETP treatment. We suggest that the damage to mitochondria is a major contributing factor involved in ETP-induced cardiotoxicity and the activation of the p53-mediated ferroptosis pathway by ETP is likely the critical pathway in ETP-induced cardiotoxicity. We also conclude that the genomic biomarkers identified in this study will significantly contribute to develop and predict potential cardiotoxic effects of novel anti-cancer drugs in vitro. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00204-018-2170-7) contains supplementary material, which is available to authorized users. Springer Berlin Heidelberg 2018-02-03 2018 /pmc/articles/PMC5882643/ /pubmed/29397400 http://dx.doi.org/10.1007/s00204-018-2170-7 Text en © The Author(s) 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided 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.
spellingShingle In Vitro Systems
Nemade, Harshal
Chaudhari, Umesh
Acharya, Aviseka
Hescheler, Jürgen
Hengstler, Jan Georg
Papadopoulos, Symeon
Sachinidis, Agapios
Cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells
title Cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells
title_full Cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells
title_fullStr Cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells
title_full_unstemmed Cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells
title_short Cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells
title_sort cell death mechanisms of the anti-cancer drug etoposide on human cardiomyocytes isolated from pluripotent stem cells
topic In Vitro Systems
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5882643/
https://www.ncbi.nlm.nih.gov/pubmed/29397400
http://dx.doi.org/10.1007/s00204-018-2170-7
work_keys_str_mv AT nemadeharshal celldeathmechanismsoftheanticancerdrugetoposideonhumancardiomyocytesisolatedfrompluripotentstemcells
AT chaudhariumesh celldeathmechanismsoftheanticancerdrugetoposideonhumancardiomyocytesisolatedfrompluripotentstemcells
AT acharyaaviseka celldeathmechanismsoftheanticancerdrugetoposideonhumancardiomyocytesisolatedfrompluripotentstemcells
AT heschelerjurgen celldeathmechanismsoftheanticancerdrugetoposideonhumancardiomyocytesisolatedfrompluripotentstemcells
AT hengstlerjangeorg celldeathmechanismsoftheanticancerdrugetoposideonhumancardiomyocytesisolatedfrompluripotentstemcells
AT papadopoulossymeon celldeathmechanismsoftheanticancerdrugetoposideonhumancardiomyocytesisolatedfrompluripotentstemcells
AT sachinidisagapios celldeathmechanismsoftheanticancerdrugetoposideonhumancardiomyocytesisolatedfrompluripotentstemcells

Ejemplares similares