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Fine-tuned KDM1A alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism

The histone demethylase KDM1A is a multi-faceted regulator of vital developmental processes, including mesodermal and cardiac tube formation during gastrulation. However, it is unknown whether the fine-tuning of KDM1A splicing isoforms, already shown to regulate neuronal maturation, is crucial for t...

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Autores principales: Astro, Veronica, Ramirez-Calderon, Gustavo, Pennucci, Roberta, Caroli, Jonatan, Saera-Vila, Alfonso, Cardona-Londoño, Kelly, Forastieri, Chiara, Fiacco, Elisabetta, Maksoud, Fatima, Alowaysi, Maryam, Sogne, Elisa, Falqui, Andrea, Gonzàlez, Federico, Montserrat, Nuria, Battaglioli, Elena, Mattevi, Andrea, Adamo, Antonio
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9287196/
https://www.ncbi.nlm.nih.gov/pubmed/35856020
http://dx.doi.org/10.1016/j.isci.2022.104665
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author Astro, Veronica
Ramirez-Calderon, Gustavo
Pennucci, Roberta
Caroli, Jonatan
Saera-Vila, Alfonso
Cardona-Londoño, Kelly
Forastieri, Chiara
Fiacco, Elisabetta
Maksoud, Fatima
Alowaysi, Maryam
Sogne, Elisa
Falqui, Andrea
Gonzàlez, Federico
Montserrat, Nuria
Battaglioli, Elena
Mattevi, Andrea
Adamo, Antonio
author_facet Astro, Veronica
Ramirez-Calderon, Gustavo
Pennucci, Roberta
Caroli, Jonatan
Saera-Vila, Alfonso
Cardona-Londoño, Kelly
Forastieri, Chiara
Fiacco, Elisabetta
Maksoud, Fatima
Alowaysi, Maryam
Sogne, Elisa
Falqui, Andrea
Gonzàlez, Federico
Montserrat, Nuria
Battaglioli, Elena
Mattevi, Andrea
Adamo, Antonio
author_sort Astro, Veronica
collection PubMed
description The histone demethylase KDM1A is a multi-faceted regulator of vital developmental processes, including mesodermal and cardiac tube formation during gastrulation. However, it is unknown whether the fine-tuning of KDM1A splicing isoforms, already shown to regulate neuronal maturation, is crucial for the specification and maintenance of cell identity during cardiogenesis. Here, we discovered a temporal modulation of ubKDM1A and KDM1A+2a during human and mice fetal cardiac development and evaluated their impact on the regulation of cardiac differentiation. We revealed a severely impaired cardiac differentiation in KDM1A(−/−) hESCs that can be rescued by re-expressing ubKDM1A or catalytically impaired ubKDM1A-K661A, but not by KDM1A+2a or KDM1A+2a-K661A. Conversely, KDM1A+2a(−/−) hESCs give rise to functional cardiac cells, displaying increased beating amplitude and frequency and enhanced expression of critical cardiogenic markers. Our findings prove the existence of a divergent scaffolding role of KDM1A splice variants, independent of their enzymatic activity, during hESC differentiation into cardiac cells.
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spelling pubmed-92871962022-07-17 Fine-tuned KDM1A alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism Astro, Veronica Ramirez-Calderon, Gustavo Pennucci, Roberta Caroli, Jonatan Saera-Vila, Alfonso Cardona-Londoño, Kelly Forastieri, Chiara Fiacco, Elisabetta Maksoud, Fatima Alowaysi, Maryam Sogne, Elisa Falqui, Andrea Gonzàlez, Federico Montserrat, Nuria Battaglioli, Elena Mattevi, Andrea Adamo, Antonio iScience Article The histone demethylase KDM1A is a multi-faceted regulator of vital developmental processes, including mesodermal and cardiac tube formation during gastrulation. However, it is unknown whether the fine-tuning of KDM1A splicing isoforms, already shown to regulate neuronal maturation, is crucial for the specification and maintenance of cell identity during cardiogenesis. Here, we discovered a temporal modulation of ubKDM1A and KDM1A+2a during human and mice fetal cardiac development and evaluated their impact on the regulation of cardiac differentiation. We revealed a severely impaired cardiac differentiation in KDM1A(−/−) hESCs that can be rescued by re-expressing ubKDM1A or catalytically impaired ubKDM1A-K661A, but not by KDM1A+2a or KDM1A+2a-K661A. Conversely, KDM1A+2a(−/−) hESCs give rise to functional cardiac cells, displaying increased beating amplitude and frequency and enhanced expression of critical cardiogenic markers. Our findings prove the existence of a divergent scaffolding role of KDM1A splice variants, independent of their enzymatic activity, during hESC differentiation into cardiac cells. Elsevier 2022-06-23 /pmc/articles/PMC9287196/ /pubmed/35856020 http://dx.doi.org/10.1016/j.isci.2022.104665 Text en © 2022 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Astro, Veronica
Ramirez-Calderon, Gustavo
Pennucci, Roberta
Caroli, Jonatan
Saera-Vila, Alfonso
Cardona-Londoño, Kelly
Forastieri, Chiara
Fiacco, Elisabetta
Maksoud, Fatima
Alowaysi, Maryam
Sogne, Elisa
Falqui, Andrea
Gonzàlez, Federico
Montserrat, Nuria
Battaglioli, Elena
Mattevi, Andrea
Adamo, Antonio
Fine-tuned KDM1A alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism
title Fine-tuned KDM1A alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism
title_full Fine-tuned KDM1A alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism
title_fullStr Fine-tuned KDM1A alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism
title_full_unstemmed Fine-tuned KDM1A alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism
title_short Fine-tuned KDM1A alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism
title_sort fine-tuned kdm1a alternative splicing regulates human cardiomyogenesis through an enzymatic-independent mechanism
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9287196/
https://www.ncbi.nlm.nih.gov/pubmed/35856020
http://dx.doi.org/10.1016/j.isci.2022.104665
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