Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia

AIMS: Human-induced pluripotent stem cell-cardiomyocytes (hiPSC-CMs) are widely used to study arrhythmia-associated mutations in ion channels. Among these, the cardiac sodium channel SCN5A undergoes foetal-to-adult isoform switching around birth. Conventional hiPSC-CM cultures, which are phenotypica...

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Autores principales: Campostrini, Giulia, Kosmidis, Georgios, Ward-van Oostwaard, Dorien, Davis, Richard Paul, Yiangou, Loukia, Ottaviani, Daniele, Veerman, Christiaan Cornelis, Mei, Hailiang, Orlova, Valeria Viktorovna, Wilde, Arthur Arnold Maria, Bezzina, Connie Rose, Verkerk, Arie Otto, Mummery, Christine Lindsay, Bellin, Milena
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10022870/
https://www.ncbi.nlm.nih.gov/pubmed/35394010
http://dx.doi.org/10.1093/cvr/cvac059
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author Campostrini, Giulia
Kosmidis, Georgios
Ward-van Oostwaard, Dorien
Davis, Richard Paul
Yiangou, Loukia
Ottaviani, Daniele
Veerman, Christiaan Cornelis
Mei, Hailiang
Orlova, Valeria Viktorovna
Wilde, Arthur Arnold Maria
Bezzina, Connie Rose
Verkerk, Arie Otto
Mummery, Christine Lindsay
Bellin, Milena
author_facet Campostrini, Giulia
Kosmidis, Georgios
Ward-van Oostwaard, Dorien
Davis, Richard Paul
Yiangou, Loukia
Ottaviani, Daniele
Veerman, Christiaan Cornelis
Mei, Hailiang
Orlova, Valeria Viktorovna
Wilde, Arthur Arnold Maria
Bezzina, Connie Rose
Verkerk, Arie Otto
Mummery, Christine Lindsay
Bellin, Milena
author_sort Campostrini, Giulia
collection PubMed
description AIMS: Human-induced pluripotent stem cell-cardiomyocytes (hiPSC-CMs) are widely used to study arrhythmia-associated mutations in ion channels. Among these, the cardiac sodium channel SCN5A undergoes foetal-to-adult isoform switching around birth. Conventional hiPSC-CM cultures, which are phenotypically foetal, have thus far been unable to capture mutations in adult gene isoforms. Here, we investigated whether tri-cellular cross-talk in a three-dimensional (3D) cardiac microtissue (MT) promoted post-natal SCN5A maturation in hiPSC-CMs. METHODS AND RESULTS: We derived patient hiPSC-CMs carrying compound mutations in the adult SCN5A exon 6B and exon 4. Electrophysiological properties of patient hiPSC-CMs in monolayer were not altered by the exon 6B mutation compared with isogenic controls since it is not expressed; further, CRISPR/Cas9-mediated excision of the foetal exon 6A did not promote adult SCN5A expression. However, when hiPSC-CMs were matured in 3D cardiac MTs, SCN5A underwent isoform switch and the functional consequences of the mutation located in exon 6B were revealed. Up-regulation of the splicing factor muscleblind-like protein 1 (MBNL1) drove SCN5A post-natal maturation in microtissues since its overexpression in hiPSC-CMs was sufficient to promote exon 6B inclusion, whilst knocking-out MBNL1 failed to foster isoform switch. CONCLUSIONS: Our study shows that (i) the tri-cellular cardiac microtissues promote post-natal SCN5A isoform switch in hiPSC-CMs, (ii) adult splicing of SCN5A is driven by MBNL1 in these tissues, and (iii) this model can be used for examining post-natal cardiac arrhythmias due to mutations in the exon 6B. TRANSLATIONAL PERSPECTIVE: The cardiac sodium channel is essential for conducting the electrical impulse in the heart. Postnatal alternative splicing regulation causes mutual exclusive inclusion of fetal or adult exons of the corresponding gene, SCN5A. Typically, immature hiPSCCMs fall short in studying the effect of mutations located in the adult exon. We describe here that an innovative tri-cellular three-dimensional cardiac microtissue culture promotes hiPSC-CMs maturation through upregulation of MBNL1, thus revealing the effect of a pathogenic genetic variant located in the SCN5A adult exon. These results help advancing the use of hiPSC-CMs in studying adult heart disease and for developing personalized medicine applications.
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spelling pubmed-100228702023-03-18 Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia Campostrini, Giulia Kosmidis, Georgios Ward-van Oostwaard, Dorien Davis, Richard Paul Yiangou, Loukia Ottaviani, Daniele Veerman, Christiaan Cornelis Mei, Hailiang Orlova, Valeria Viktorovna Wilde, Arthur Arnold Maria Bezzina, Connie Rose Verkerk, Arie Otto Mummery, Christine Lindsay Bellin, Milena Cardiovasc Res Original Article AIMS: Human-induced pluripotent stem cell-cardiomyocytes (hiPSC-CMs) are widely used to study arrhythmia-associated mutations in ion channels. Among these, the cardiac sodium channel SCN5A undergoes foetal-to-adult isoform switching around birth. Conventional hiPSC-CM cultures, which are phenotypically foetal, have thus far been unable to capture mutations in adult gene isoforms. Here, we investigated whether tri-cellular cross-talk in a three-dimensional (3D) cardiac microtissue (MT) promoted post-natal SCN5A maturation in hiPSC-CMs. METHODS AND RESULTS: We derived patient hiPSC-CMs carrying compound mutations in the adult SCN5A exon 6B and exon 4. Electrophysiological properties of patient hiPSC-CMs in monolayer were not altered by the exon 6B mutation compared with isogenic controls since it is not expressed; further, CRISPR/Cas9-mediated excision of the foetal exon 6A did not promote adult SCN5A expression. However, when hiPSC-CMs were matured in 3D cardiac MTs, SCN5A underwent isoform switch and the functional consequences of the mutation located in exon 6B were revealed. Up-regulation of the splicing factor muscleblind-like protein 1 (MBNL1) drove SCN5A post-natal maturation in microtissues since its overexpression in hiPSC-CMs was sufficient to promote exon 6B inclusion, whilst knocking-out MBNL1 failed to foster isoform switch. CONCLUSIONS: Our study shows that (i) the tri-cellular cardiac microtissues promote post-natal SCN5A isoform switch in hiPSC-CMs, (ii) adult splicing of SCN5A is driven by MBNL1 in these tissues, and (iii) this model can be used for examining post-natal cardiac arrhythmias due to mutations in the exon 6B. TRANSLATIONAL PERSPECTIVE: The cardiac sodium channel is essential for conducting the electrical impulse in the heart. Postnatal alternative splicing regulation causes mutual exclusive inclusion of fetal or adult exons of the corresponding gene, SCN5A. Typically, immature hiPSCCMs fall short in studying the effect of mutations located in the adult exon. We describe here that an innovative tri-cellular three-dimensional cardiac microtissue culture promotes hiPSC-CMs maturation through upregulation of MBNL1, thus revealing the effect of a pathogenic genetic variant located in the SCN5A adult exon. These results help advancing the use of hiPSC-CMs in studying adult heart disease and for developing personalized medicine applications. Oxford University Press 2022-04-08 /pmc/articles/PMC10022870/ /pubmed/35394010 http://dx.doi.org/10.1093/cvr/cvac059 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of the European Society of Cardiology. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Article
Campostrini, Giulia
Kosmidis, Georgios
Ward-van Oostwaard, Dorien
Davis, Richard Paul
Yiangou, Loukia
Ottaviani, Daniele
Veerman, Christiaan Cornelis
Mei, Hailiang
Orlova, Valeria Viktorovna
Wilde, Arthur Arnold Maria
Bezzina, Connie Rose
Verkerk, Arie Otto
Mummery, Christine Lindsay
Bellin, Milena
Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia
title Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia
title_full Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia
title_fullStr Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia
title_full_unstemmed Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia
title_short Maturation of hiPSC-derived cardiomyocytes promotes adult alternative splicing of SCN5A and reveals changes in sodium current associated with cardiac arrhythmia
title_sort maturation of hipsc-derived cardiomyocytes promotes adult alternative splicing of scn5a and reveals changes in sodium current associated with cardiac arrhythmia
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10022870/
https://www.ncbi.nlm.nih.gov/pubmed/35394010
http://dx.doi.org/10.1093/cvr/cvac059
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