Late sodium current inhibition reverses electromechanical dysfunction in human hypertrophic cardiomyopathy

Raffaele Coppini; Cecilia Ferrantini; Lina Yao; Peidong Fan; Martina Del Lungo; Francesca Stillitano; Laura Sartiani; Benedetta Tosi; Silvia Suffredini; Chiara Tesi; Magdi Yacoub; Iacopo Olivotto; Luiz Belardinelli; Corrado Poggesi; Elisabetta Cerbai; Alessandro Mugelli

doi:10.1161/CIRCULATIONAHA.112.134932

Late sodium current inhibition reverses electromechanical dysfunction in human hypertrophic cardiomyopathy

Raffaele Coppini^*, Cecilia Ferrantini, Lina Yao, Peidong Fan, Martina Del Lungo, Francesca Stillitano, Laura Sartiani, Benedetta Tosi, Silvia Suffredini, Chiara Tesi, Magdi Yacoub, Iacopo Olivotto, Luiz Belardinelli, Corrado Poggesi, Elisabetta Cerbai, Alessandro Mugelli

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

BACKGROUND-: Hypertrophic cardiomyopathy (HCM), the most common mendelian heart disorder, remains an orphan of disease-specific pharmacological treatment because of the limited understanding of cellular mechanisms underlying arrhythmogenicity and diastolic dysfunction. METHODS AND RESULTS-: We assessed the electromechanical profile of cardiomyocytes from 26 HCM patients undergoing myectomy compared with those from nonfailing nonhypertrophic surgical patients by performing patch-clamp and intracellular Ca (Cai) studies. Compared with controls, HCM cardiomyocytes showed prolonged action potential related to increased late Na (INaL) and Ca (ICaL) currents and decreased repolarizing K currents, increased occurrence of cellular arrhythmias, prolonged Cai transients, and higher diastolic Cai. Such changes were related to enhanced Ca/calmodulin kinase II (CaMKII) activity and increased phosphorylation of its targets. Ranolazine at therapeutic concentrations partially reversed the HCM-related cellular abnormalities via INaL inhibition, with negligible effects in controls. By shortening the action potential duration in HCM cardiomyocytes, ranolazine reduced the occurrence of early and delayed afterdepolarizations. Finally, as a result of the faster kinetics of Cai transients and the lower diastolic Cai, ranolazine accelerated the contraction-relaxation cycle of HCM trabeculae, ameliorating diastolic function. CONCLUSIONS-: We highlighted a specific set of functional changes in human HCM myocardium that stem from a complex remodeling process involving alterations of CaMKII-dependent signaling, rather than being a direct consequence of the causal sarcomeric mutations. Among the several ion channel and Cai handling proteins changes identified, an enhanced INaL seems to be a major contributor to the electrophysiological and Cai dynamic abnormalities of ventricular myocytes and trabeculae from patients with HCM, suggesting potential therapeutic implications of INaL inhibition.

Original language	English
Pages (from-to)	575-584
Number of pages	10
Journal	Circulation
Volume	127
Issue number	5
DOIs	https://doi.org/10.1161/CIRCULATIONAHA.112.134932
Publication status	Published - 5 Feb 2013
Externally published	Yes

Keywords

Action potentials
arrhythmias, cardiac
diastole
hypertrophy
myocytes, cardiac

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10.1161/CIRCULATIONAHA.112.134932

Cite this

Coppini, R., Ferrantini, C., Yao, L., Fan, P., Del Lungo, M., Stillitano, F., Sartiani, L., Tosi, B., Suffredini, S., Tesi, C., Yacoub, M., Olivotto, I., Belardinelli, L., Poggesi, C., Cerbai, E., & Mugelli, A. (2013). Late sodium current inhibition reverses electromechanical dysfunction in human hypertrophic cardiomyopathy. Circulation, 127(5), 575-584. https://doi.org/10.1161/CIRCULATIONAHA.112.134932

@article{a449a3fd672a4a719c5ce57caa119094,

title = "Late sodium current inhibition reverses electromechanical dysfunction in human hypertrophic cardiomyopathy",

abstract = "BACKGROUND-: Hypertrophic cardiomyopathy (HCM), the most common mendelian heart disorder, remains an orphan of disease-specific pharmacological treatment because of the limited understanding of cellular mechanisms underlying arrhythmogenicity and diastolic dysfunction. METHODS AND RESULTS-: We assessed the electromechanical profile of cardiomyocytes from 26 HCM patients undergoing myectomy compared with those from nonfailing nonhypertrophic surgical patients by performing patch-clamp and intracellular Ca (Cai) studies. Compared with controls, HCM cardiomyocytes showed prolonged action potential related to increased late Na (INaL) and Ca (ICaL) currents and decreased repolarizing K currents, increased occurrence of cellular arrhythmias, prolonged Cai transients, and higher diastolic Cai. Such changes were related to enhanced Ca/calmodulin kinase II (CaMKII) activity and increased phosphorylation of its targets. Ranolazine at therapeutic concentrations partially reversed the HCM-related cellular abnormalities via INaL inhibition, with negligible effects in controls. By shortening the action potential duration in HCM cardiomyocytes, ranolazine reduced the occurrence of early and delayed afterdepolarizations. Finally, as a result of the faster kinetics of Cai transients and the lower diastolic Cai, ranolazine accelerated the contraction-relaxation cycle of HCM trabeculae, ameliorating diastolic function. CONCLUSIONS-: We highlighted a specific set of functional changes in human HCM myocardium that stem from a complex remodeling process involving alterations of CaMKII-dependent signaling, rather than being a direct consequence of the causal sarcomeric mutations. Among the several ion channel and Cai handling proteins changes identified, an enhanced INaL seems to be a major contributor to the electrophysiological and Cai dynamic abnormalities of ventricular myocytes and trabeculae from patients with HCM, suggesting potential therapeutic implications of INaL inhibition.",

keywords = "Action potentials, arrhythmias, cardiac, diastole, hypertrophy, myocytes, cardiac",

author = "Raffaele Coppini and Cecilia Ferrantini and Lina Yao and Peidong Fan and {Del Lungo}, Martina and Francesca Stillitano and Laura Sartiani and Benedetta Tosi and Silvia Suffredini and Chiara Tesi and Magdi Yacoub and Iacopo Olivotto and Luiz Belardinelli and Corrado Poggesi and Elisabetta Cerbai and Alessandro Mugelli",

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doi = "10.1161/CIRCULATIONAHA.112.134932",

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Coppini, R, Ferrantini, C, Yao, L, Fan, P, Del Lungo, M, Stillitano, F, Sartiani, L, Tosi, B, Suffredini, S, Tesi, C, Yacoub, M, Olivotto, I, Belardinelli, L, Poggesi, C, Cerbai, E & Mugelli, A 2013, 'Late sodium current inhibition reverses electromechanical dysfunction in human hypertrophic cardiomyopathy', Circulation, vol. 127, no. 5, pp. 575-584. https://doi.org/10.1161/CIRCULATIONAHA.112.134932

TY - JOUR

T1 - Late sodium current inhibition reverses electromechanical dysfunction in human hypertrophic cardiomyopathy

AU - Coppini, Raffaele

AU - Ferrantini, Cecilia

AU - Yao, Lina

AU - Fan, Peidong

AU - Del Lungo, Martina

AU - Stillitano, Francesca

AU - Sartiani, Laura

AU - Tosi, Benedetta

AU - Suffredini, Silvia

AU - Tesi, Chiara

AU - Yacoub, Magdi

AU - Olivotto, Iacopo

AU - Belardinelli, Luiz

AU - Poggesi, Corrado

AU - Cerbai, Elisabetta

AU - Mugelli, Alessandro

PY - 2013/2/5

Y1 - 2013/2/5

N2 - BACKGROUND-: Hypertrophic cardiomyopathy (HCM), the most common mendelian heart disorder, remains an orphan of disease-specific pharmacological treatment because of the limited understanding of cellular mechanisms underlying arrhythmogenicity and diastolic dysfunction. METHODS AND RESULTS-: We assessed the electromechanical profile of cardiomyocytes from 26 HCM patients undergoing myectomy compared with those from nonfailing nonhypertrophic surgical patients by performing patch-clamp and intracellular Ca (Cai) studies. Compared with controls, HCM cardiomyocytes showed prolonged action potential related to increased late Na (INaL) and Ca (ICaL) currents and decreased repolarizing K currents, increased occurrence of cellular arrhythmias, prolonged Cai transients, and higher diastolic Cai. Such changes were related to enhanced Ca/calmodulin kinase II (CaMKII) activity and increased phosphorylation of its targets. Ranolazine at therapeutic concentrations partially reversed the HCM-related cellular abnormalities via INaL inhibition, with negligible effects in controls. By shortening the action potential duration in HCM cardiomyocytes, ranolazine reduced the occurrence of early and delayed afterdepolarizations. Finally, as a result of the faster kinetics of Cai transients and the lower diastolic Cai, ranolazine accelerated the contraction-relaxation cycle of HCM trabeculae, ameliorating diastolic function. CONCLUSIONS-: We highlighted a specific set of functional changes in human HCM myocardium that stem from a complex remodeling process involving alterations of CaMKII-dependent signaling, rather than being a direct consequence of the causal sarcomeric mutations. Among the several ion channel and Cai handling proteins changes identified, an enhanced INaL seems to be a major contributor to the electrophysiological and Cai dynamic abnormalities of ventricular myocytes and trabeculae from patients with HCM, suggesting potential therapeutic implications of INaL inhibition.

AB - BACKGROUND-: Hypertrophic cardiomyopathy (HCM), the most common mendelian heart disorder, remains an orphan of disease-specific pharmacological treatment because of the limited understanding of cellular mechanisms underlying arrhythmogenicity and diastolic dysfunction. METHODS AND RESULTS-: We assessed the electromechanical profile of cardiomyocytes from 26 HCM patients undergoing myectomy compared with those from nonfailing nonhypertrophic surgical patients by performing patch-clamp and intracellular Ca (Cai) studies. Compared with controls, HCM cardiomyocytes showed prolonged action potential related to increased late Na (INaL) and Ca (ICaL) currents and decreased repolarizing K currents, increased occurrence of cellular arrhythmias, prolonged Cai transients, and higher diastolic Cai. Such changes were related to enhanced Ca/calmodulin kinase II (CaMKII) activity and increased phosphorylation of its targets. Ranolazine at therapeutic concentrations partially reversed the HCM-related cellular abnormalities via INaL inhibition, with negligible effects in controls. By shortening the action potential duration in HCM cardiomyocytes, ranolazine reduced the occurrence of early and delayed afterdepolarizations. Finally, as a result of the faster kinetics of Cai transients and the lower diastolic Cai, ranolazine accelerated the contraction-relaxation cycle of HCM trabeculae, ameliorating diastolic function. CONCLUSIONS-: We highlighted a specific set of functional changes in human HCM myocardium that stem from a complex remodeling process involving alterations of CaMKII-dependent signaling, rather than being a direct consequence of the causal sarcomeric mutations. Among the several ion channel and Cai handling proteins changes identified, an enhanced INaL seems to be a major contributor to the electrophysiological and Cai dynamic abnormalities of ventricular myocytes and trabeculae from patients with HCM, suggesting potential therapeutic implications of INaL inhibition.

KW - Action potentials

KW - arrhythmias, cardiac

KW - diastole

KW - hypertrophy

KW - myocytes, cardiac

UR - http://www.scopus.com/inward/record.url?scp=84873567647&partnerID=8YFLogxK

U2 - 10.1161/CIRCULATIONAHA.112.134932

DO - 10.1161/CIRCULATIONAHA.112.134932

M3 - Article

C2 - 23271797

AN - SCOPUS:84873567647

SN - 0009-7322

VL - 127

SP - 575

EP - 584

JO - Circulation

JF - Circulation

IS - 5

ER -

Late sodium current inhibition reverses electromechanical dysfunction in human hypertrophic cardiomyopathy

Abstract

Keywords

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