Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.

Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.

Executioner caspase-3 and -7 are proteases promoting cell death but non-apoptotic roles are being discovered. The heart expresses caspases only during development, suggesting they contribute to the organ maturation process. Therefore, we aimed at identifying novel functions of caspases in heart deve...

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Main Authors: Maria Cardona, Juan Antonio López, Anna Serafín, Anthony Rongvaux, Javier Inserte, David García-Dorado, Richard Flavell, Marta Llovera, Xavier Cañas, Jesús Vázquez, Daniel Sanchis
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4487935?pdf=render
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spelling doaj-7b0ee7ead6124cd094228c2fbc76412f2020-11-24T21:10:44ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01106e013141110.1371/journal.pone.0131411Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.Maria CardonaJuan Antonio LópezAnna SerafínAnthony RongvauxJavier InserteDavid García-DoradoRichard FlavellMarta LloveraXavier CañasJesús VázquezDaniel SanchisExecutioner caspase-3 and -7 are proteases promoting cell death but non-apoptotic roles are being discovered. The heart expresses caspases only during development, suggesting they contribute to the organ maturation process. Therefore, we aimed at identifying novel functions of caspases in heart development. We induced simultaneous deletion of executioner caspase-3 and -7 in the mouse myocardium and studied its effects. Caspase knockout hearts are hypoplastic at birth, reaching normal weight progressively through myocyte hypertrophy. To identify the molecular pathways involved in these effects, we used microarray-based transcriptomics and multiplexed quantitative proteomics to compare wild type and executioner caspase-deficient myocardium at different developmental stages. Transcriptomics showed reduced expression of genes promoting DNA replication and cell cycle progression in the neonatal caspase-deficient heart suggesting reduced myocyte proliferation, and expression of non-cardiac isoforms of structural proteins in the adult null myocardium. Proteomics showed reduced abundance of proteins involved in oxidative phosphorylation accompanied by increased abundance of glycolytic enzymes underscoring retarded metabolic maturation of the caspase-null myocardium. Correlation between mRNA expression and protein abundance of relevant genes was confirmed, but transcriptomics and proteomics indentified complementary molecular pathways influenced by caspases in the developing heart. Forced expression of wild type or proteolytically inactive caspases in cultured cardiomyocytes induced expression of genes promoting cell division. The results reveal that executioner caspases can modulate heart's cellularity and maturation during development, contributing novel information about caspase biology and heart development.http://europepmc.org/articles/PMC4487935?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Maria Cardona
Juan Antonio López
Anna Serafín
Anthony Rongvaux
Javier Inserte
David García-Dorado
Richard Flavell
Marta Llovera
Xavier Cañas
Jesús Vázquez
Daniel Sanchis
spellingShingle Maria Cardona
Juan Antonio López
Anna Serafín
Anthony Rongvaux
Javier Inserte
David García-Dorado
Richard Flavell
Marta Llovera
Xavier Cañas
Jesús Vázquez
Daniel Sanchis
Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.
PLoS ONE
author_facet Maria Cardona
Juan Antonio López
Anna Serafín
Anthony Rongvaux
Javier Inserte
David García-Dorado
Richard Flavell
Marta Llovera
Xavier Cañas
Jesús Vázquez
Daniel Sanchis
author_sort Maria Cardona
title Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.
title_short Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.
title_full Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.
title_fullStr Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.
title_full_unstemmed Executioner Caspase-3 and 7 Deficiency Reduces Myocyte Number in the Developing Mouse Heart.
title_sort executioner caspase-3 and 7 deficiency reduces myocyte number in the developing mouse heart.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description Executioner caspase-3 and -7 are proteases promoting cell death but non-apoptotic roles are being discovered. The heart expresses caspases only during development, suggesting they contribute to the organ maturation process. Therefore, we aimed at identifying novel functions of caspases in heart development. We induced simultaneous deletion of executioner caspase-3 and -7 in the mouse myocardium and studied its effects. Caspase knockout hearts are hypoplastic at birth, reaching normal weight progressively through myocyte hypertrophy. To identify the molecular pathways involved in these effects, we used microarray-based transcriptomics and multiplexed quantitative proteomics to compare wild type and executioner caspase-deficient myocardium at different developmental stages. Transcriptomics showed reduced expression of genes promoting DNA replication and cell cycle progression in the neonatal caspase-deficient heart suggesting reduced myocyte proliferation, and expression of non-cardiac isoforms of structural proteins in the adult null myocardium. Proteomics showed reduced abundance of proteins involved in oxidative phosphorylation accompanied by increased abundance of glycolytic enzymes underscoring retarded metabolic maturation of the caspase-null myocardium. Correlation between mRNA expression and protein abundance of relevant genes was confirmed, but transcriptomics and proteomics indentified complementary molecular pathways influenced by caspases in the developing heart. Forced expression of wild type or proteolytically inactive caspases in cultured cardiomyocytes induced expression of genes promoting cell division. The results reveal that executioner caspases can modulate heart's cellularity and maturation during development, contributing novel information about caspase biology and heart development.
url http://europepmc.org/articles/PMC4487935?pdf=render
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