Slower Calcium Handling Balances Faster Cross-Bridge Cycling in Human MYBPC3 HCM

The pathogenesis of MYBPC3-associated hypertrophic cardiomyopathy (HCM) is still unresolved. In our HCM patient cohort, a large and well-characterized population carrying the MYBPC3:c772G>A variant (p.Glu258Lys, E258K) provides the unique opportunity to study the basic mechanisms of MYBPC3-HCM wi...

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Autores principales: Pioner, Josè Manuel, Vitale, Giulia, Steczina, Sonette, Langione, Marianna, Margara, Francesca, Santini, Lorenzo, Giardini, Francesco, Lazzeri, Erica, Piroddi, Nicoletta, Scellini, Beatrice, Palandri, Chiara, Schuldt, Maike, Spinelli, Valentina, Girolami, Francesca, Mazzarotto, Francesco, van der Velden, Jolanda, Cerbai, Elisabetta, Tesi, Chiara, Olivotto, Iacopo, Bueno-Orovio, Alfonso, Sacconi, Leonardo, Coppini, Raffaele, Ferrantini, Cecilia, Regnier, Michael, Poggesi, Corrado
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Lippincott Williams & Wilkins 2023
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9977265/
https://www.ncbi.nlm.nih.gov/pubmed/36744470
http://dx.doi.org/10.1161/CIRCRESAHA.122.321956
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author Pioner, Josè Manuel
Vitale, Giulia
Steczina, Sonette
Langione, Marianna
Margara, Francesca
Santini, Lorenzo
Giardini, Francesco
Lazzeri, Erica
Piroddi, Nicoletta
Scellini, Beatrice
Palandri, Chiara
Schuldt, Maike
Spinelli, Valentina
Girolami, Francesca
Mazzarotto, Francesco
van der Velden, Jolanda
Cerbai, Elisabetta
Tesi, Chiara
Olivotto, Iacopo
Bueno-Orovio, Alfonso
Sacconi, Leonardo
Coppini, Raffaele
Ferrantini, Cecilia
Regnier, Michael
Poggesi, Corrado
author_facet Pioner, Josè Manuel
Vitale, Giulia
Steczina, Sonette
Langione, Marianna
Margara, Francesca
Santini, Lorenzo
Giardini, Francesco
Lazzeri, Erica
Piroddi, Nicoletta
Scellini, Beatrice
Palandri, Chiara
Schuldt, Maike
Spinelli, Valentina
Girolami, Francesca
Mazzarotto, Francesco
van der Velden, Jolanda
Cerbai, Elisabetta
Tesi, Chiara
Olivotto, Iacopo
Bueno-Orovio, Alfonso
Sacconi, Leonardo
Coppini, Raffaele
Ferrantini, Cecilia
Regnier, Michael
Poggesi, Corrado
author_sort Pioner, Josè Manuel
collection PubMed
description The pathogenesis of MYBPC3-associated hypertrophic cardiomyopathy (HCM) is still unresolved. In our HCM patient cohort, a large and well-characterized population carrying the MYBPC3:c772G>A variant (p.Glu258Lys, E258K) provides the unique opportunity to study the basic mechanisms of MYBPC3-HCM with a comprehensive translational approach. METHODS: We collected clinical and genetic data from 93 HCM patients carrying the MYBPC3:c772G>A variant. Functional perturbations were investigated using different biophysical techniques in left ventricular samples from 4 patients who underwent myectomy for refractory outflow obstruction, compared with samples from non-failing non-hypertrophic surgical patients and healthy donors. Human induced pluripotent stem cell (hiPSC)-derived cardiomyocytes and engineered heart tissues (EHTs) were also investigated. RESULTS: Haplotype analysis revealed MYBPC3:c772G>A as a founder mutation in Tuscany. In ventricular myocardium, the mutation leads to reduced cMyBP-C (cardiac myosin binding protein-C) expression, supporting haploinsufficiency as the main primary disease mechanism. Mechanical studies in single myofibrils and permeabilized muscle strips highlighted faster cross-bridge cycling, and higher energy cost of tension generation. A novel approach based on tissue clearing and advanced optical microscopy supported the idea that the sarcomere energetics dysfunction is intrinsically related with the reduction in cMyBP-C. Studies in single cardiomyocytes (native and hiPSC-derived), intact trabeculae and hiPSC-EHTs revealed prolonged action potentials, slower Ca(2+) transients and preserved twitch duration, suggesting that the slower excitation-contraction coupling counterbalanced the faster sarcomere kinetics. This conclusion was strengthened by in silico simulations. CONCLUSIONS: HCM-related MYBPC3:c772G>A mutation invariably impairs sarcomere energetics and cross-bridge cycling. Compensatory electrophysiological changes (eg, reduced potassium channel expression) appear to preserve twitch contraction parameters, but may expose patients to greater arrhythmic propensity and disease progression. Therapeutic approaches correcting the primary sarcomeric defects may prevent secondary cardiomyocyte remodeling.
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spelling pubmed-99772652023-03-02 Slower Calcium Handling Balances Faster Cross-Bridge Cycling in Human MYBPC3 HCM Pioner, Josè Manuel Vitale, Giulia Steczina, Sonette Langione, Marianna Margara, Francesca Santini, Lorenzo Giardini, Francesco Lazzeri, Erica Piroddi, Nicoletta Scellini, Beatrice Palandri, Chiara Schuldt, Maike Spinelli, Valentina Girolami, Francesca Mazzarotto, Francesco van der Velden, Jolanda Cerbai, Elisabetta Tesi, Chiara Olivotto, Iacopo Bueno-Orovio, Alfonso Sacconi, Leonardo Coppini, Raffaele Ferrantini, Cecilia Regnier, Michael Poggesi, Corrado Circ Res Original Research The pathogenesis of MYBPC3-associated hypertrophic cardiomyopathy (HCM) is still unresolved. In our HCM patient cohort, a large and well-characterized population carrying the MYBPC3:c772G>A variant (p.Glu258Lys, E258K) provides the unique opportunity to study the basic mechanisms of MYBPC3-HCM with a comprehensive translational approach. METHODS: We collected clinical and genetic data from 93 HCM patients carrying the MYBPC3:c772G>A variant. Functional perturbations were investigated using different biophysical techniques in left ventricular samples from 4 patients who underwent myectomy for refractory outflow obstruction, compared with samples from non-failing non-hypertrophic surgical patients and healthy donors. Human induced pluripotent stem cell (hiPSC)-derived cardiomyocytes and engineered heart tissues (EHTs) were also investigated. RESULTS: Haplotype analysis revealed MYBPC3:c772G>A as a founder mutation in Tuscany. In ventricular myocardium, the mutation leads to reduced cMyBP-C (cardiac myosin binding protein-C) expression, supporting haploinsufficiency as the main primary disease mechanism. Mechanical studies in single myofibrils and permeabilized muscle strips highlighted faster cross-bridge cycling, and higher energy cost of tension generation. A novel approach based on tissue clearing and advanced optical microscopy supported the idea that the sarcomere energetics dysfunction is intrinsically related with the reduction in cMyBP-C. Studies in single cardiomyocytes (native and hiPSC-derived), intact trabeculae and hiPSC-EHTs revealed prolonged action potentials, slower Ca(2+) transients and preserved twitch duration, suggesting that the slower excitation-contraction coupling counterbalanced the faster sarcomere kinetics. This conclusion was strengthened by in silico simulations. CONCLUSIONS: HCM-related MYBPC3:c772G>A mutation invariably impairs sarcomere energetics and cross-bridge cycling. Compensatory electrophysiological changes (eg, reduced potassium channel expression) appear to preserve twitch contraction parameters, but may expose patients to greater arrhythmic propensity and disease progression. Therapeutic approaches correcting the primary sarcomeric defects may prevent secondary cardiomyocyte remodeling. Lippincott Williams & Wilkins 2023-02-06 2023-03-03 /pmc/articles/PMC9977265/ /pubmed/36744470 http://dx.doi.org/10.1161/CIRCRESAHA.122.321956 Text en © 2023 The Authors. https://creativecommons.org/licenses/by/4.0/Circulation Research is published on behalf of the American Heart Association, Inc., by Wolters Kluwer Health, Inc. This is an open access article under the terms of the Creative Commons Attribution (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution, and reproduction in any medium, provided that the original work is properly cited. This article is made available via the PMC Open Access Subset for unrestricted re-use and analyses in any form or by any means with acknowledgement of the original source. These permissions are granted for the duration of the COVID-19 pandemic or until permissions are revoked in writing. Upon expiration of these permissions, PMC is granted a perpetual license to make this article available via PMC and Europe PMC, consistent with existing copyright protections.
spellingShingle Original Research
Pioner, Josè Manuel
Vitale, Giulia
Steczina, Sonette
Langione, Marianna
Margara, Francesca
Santini, Lorenzo
Giardini, Francesco
Lazzeri, Erica
Piroddi, Nicoletta
Scellini, Beatrice
Palandri, Chiara
Schuldt, Maike
Spinelli, Valentina
Girolami, Francesca
Mazzarotto, Francesco
van der Velden, Jolanda
Cerbai, Elisabetta
Tesi, Chiara
Olivotto, Iacopo
Bueno-Orovio, Alfonso
Sacconi, Leonardo
Coppini, Raffaele
Ferrantini, Cecilia
Regnier, Michael
Poggesi, Corrado
Slower Calcium Handling Balances Faster Cross-Bridge Cycling in Human MYBPC3 HCM
title Slower Calcium Handling Balances Faster Cross-Bridge Cycling in Human MYBPC3 HCM
title_full Slower Calcium Handling Balances Faster Cross-Bridge Cycling in Human MYBPC3 HCM
title_fullStr Slower Calcium Handling Balances Faster Cross-Bridge Cycling in Human MYBPC3 HCM
title_full_unstemmed Slower Calcium Handling Balances Faster Cross-Bridge Cycling in Human MYBPC3 HCM
title_short Slower Calcium Handling Balances Faster Cross-Bridge Cycling in Human MYBPC3 HCM
title_sort slower calcium handling balances faster cross-bridge cycling in human mybpc3 hcm
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9977265/
https://www.ncbi.nlm.nih.gov/pubmed/36744470
http://dx.doi.org/10.1161/CIRCRESAHA.122.321956
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