SCN10A-short gene therapy to restore conduction and protect against malignant cardiac arrhythmias

Jianan Wang; Arie O. Verkerk; Ronald Wilders; Yingnan Zhang; Kelly Zhang; Adityo Prakosa; Mathilde R. Rivaud; E. Madelief J. Marsman; Arie R. Boender; Mischa Klerk; Lianne Fokkert; Berend de Jonge; Klaus Neef; Osne F. Kirzner; Connie R. Bezzina; Carol Ann Remme; Hanno L. Tan; Bastiaan J. Boukens; Harsha D. Devalla; Natalia A. Trayanova; Vincent M. Christoffels; Phil Barnett; Gerard J. J. Boink

doi:10.1093/eurheartj/ehaf053

SCN10A-short gene therapy to restore conduction and protect against malignant cardiac arrhythmias

Jianan Wang
, Arie O. Verkerk
, Ronald Wilders
, Yingnan Zhang
, Kelly Zhang
, Adityo Prakosa
, Mathilde R. Rivaud
, E. Madelief J. Marsman
, Arie R. Boender
, Mischa Klerk
, Lianne Fokkert
, Berend de Jonge
, Klaus Neef
, Osne F. Kirzner
, Connie R. Bezzina
, Carol Ann Remme
, Hanno L. Tan
, Bastiaan J. Boukens
, Harsha D. Devalla
, Natalia A. Trayanova

Vincent M. Christoffels, Phil Barnett^*, Gerard J. J. Boink^*

^*Corresponding author for this work

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

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Abstract

Background and Aims Life-threatening arrhythmias are a well-established consequence of reduced cardiac sodium current (INa). Gene therapy approaches to increase INa have demonstrated potential benefits to prevent arrhythmias. However, the development of such therapies is hampered by the large size of sodium channels. In this study, SCN10A-short (S10s), a short transcript encoding the carboxy-terminal domain of the human neuronal sodium channel, was evaluated as a gene therapy target to increase INa and prevent arrhythmias. Methods Adeno-associated viral vector overexpressing S10s was injected into wild type and Scn5a-haploinsufficient mice on which patch-clamp studies, optical mapping, electrocardiogram analyses, and ischaemia reperfusion were performed.In vitro and in silico studies were conducted to further explore the effect of S10s gene therapy in the context of human hearts. Results Cardiac S10s overexpression increased cellular INa, maximal action potential upstroke velocity, and action potential amplitude in Scn5a-haploinsufficient cardiomyocytes.S10s gene therapy rescues conduction slowing in Scn5a-haploinsufficient mice and prevented ventricular tachycardia induced by ischaemia-reperfusion in wild type mice.S10s overexpression increased maximal action potential upstroke velocity in human inducible pluripotent stem cell-derived cardiomyocytes and prevented inducible arrhythmias in simulated human heart models. Conclusions S10s gene therapy may be effective to treat cardiac conduction abnormalities and associated arrhythmias.

Original language	English
Pages (from-to)	1747-1762
Number of pages	16
Journal	European heart journal
Volume	46
Issue number	18
DOIs	https://doi.org/10.1093/eurheartj/ehaf053
Publication status	Published - 7 May 2025

Keywords

AAV
Cardiac arrhythmia
Gene therapy
SCN10A
SCN5A
Sodium current

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1093/eurheartj/ehaf053

Scn10a-short-gene-therapy-to-restore-conduction-and-protect-against-malignant-cardiac-arrhythmias.pdfFinal published version, 1.81 MBLicence: CC BY

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Wang, J., Verkerk, A. O., Wilders, R., Zhang, Y., Zhang, K., Prakosa, A., Rivaud, M. R., Marsman, E. M. J., Boender, A. R., Klerk, M., Fokkert, L., de Jonge, B., Neef, K., Kirzner, O. F., Bezzina, C. R., Remme, C. A., Tan, H. L., Boukens, B. J., Devalla, H. D., ... Boink, G. J. J. (2025). SCN10A-short gene therapy to restore conduction and protect against malignant cardiac arrhythmias. European heart journal, 46(18), 1747-1762. https://doi.org/10.1093/eurheartj/ehaf053

@article{2e5177bac3594376849c371b220592bb,

title = "SCN10A-short gene therapy to restore conduction and protect against malignant cardiac arrhythmias",

abstract = "Background and Aims Life-threatening arrhythmias are a well-established consequence of reduced cardiac sodium current (INa). Gene therapy approaches to increase INa have demonstrated potential benefits to prevent arrhythmias. However, the development of such therapies is hampered by the large size of sodium channels. In this study, SCN10A-short (S10s), a short transcript encoding the carboxy-terminal domain of the human neuronal sodium channel, was evaluated as a gene therapy target to increase INa and prevent arrhythmias. Methods Adeno-associated viral vector overexpressing S10s was injected into wild type and Scn5a-haploinsufficient mice on which patch-clamp studies, optical mapping, electrocardiogram analyses, and ischaemia reperfusion were performed.In vitro and in silico studies were conducted to further explore the effect of S10s gene therapy in the context of human hearts. Results Cardiac S10s overexpression increased cellular INa, maximal action potential upstroke velocity, and action potential amplitude in Scn5a-haploinsufficient cardiomyocytes.S10s gene therapy rescues conduction slowing in Scn5a-haploinsufficient mice and prevented ventricular tachycardia induced by ischaemia-reperfusion in wild type mice.S10s overexpression increased maximal action potential upstroke velocity in human inducible pluripotent stem cell-derived cardiomyocytes and prevented inducible arrhythmias in simulated human heart models. Conclusions S10s gene therapy may be effective to treat cardiac conduction abnormalities and associated arrhythmias.",

keywords = "AAV, Cardiac arrhythmia, Gene therapy, SCN10A, SCN5A, Sodium current",

author = "Jianan Wang and Verkerk, \{Arie O.\} and Ronald Wilders and Yingnan Zhang and Kelly Zhang and Adityo Prakosa and Rivaud, \{Mathilde R.\} and Marsman, \{E. Madelief J.\} and Boender, \{Arie R.\} and Mischa Klerk and Lianne Fokkert and \{de Jonge\}, Berend and Klaus Neef and Kirzner, \{Osne F.\} and Bezzina, \{Connie R.\} and Remme, \{Carol Ann\} and Tan, \{Hanno L.\} and Boukens, \{Bastiaan J.\} and Devalla, \{Harsha D.\} and Trayanova, \{Natalia A.\} and Christoffels, \{Vincent M.\} and Phil Barnett and Boink, \{Gerard J. J.\}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025. Published by Oxford University Press on behalf of the European Society of Cardiology.",

year = "2025",

month = may,

day = "7",

doi = "10.1093/eurheartj/ehaf053",

language = "English",

volume = "46",

pages = "1747--1762",

journal = "European heart journal",

issn = "0195-668X",

publisher = "Oxford University Press",

number = "18",

}

Wang, J , Verkerk, AO , Wilders, R, Zhang, Y, Zhang, K, Prakosa, A, Rivaud, MR, Marsman, EMJ, Boender, AR, Klerk, M , Fokkert, L, de Jonge, B, Neef, K , Kirzner, OF , Bezzina, CR , Remme, CA , Tan, HL , Boukens, BJ , Devalla, HD, Trayanova, NA, Christoffels, VM , Barnett, P & Boink, GJJ 2025, 'SCN10A-short gene therapy to restore conduction and protect against malignant cardiac arrhythmias', European heart journal, vol. 46, no. 18, pp. 1747-1762. https://doi.org/10.1093/eurheartj/ehaf053

TY - JOUR

T1 - SCN10A-short gene therapy to restore conduction and protect against malignant cardiac arrhythmias

AU - Wang, Jianan

AU - Verkerk, Arie O.

AU - Wilders, Ronald

AU - Zhang, Yingnan

AU - Zhang, Kelly

AU - Prakosa, Adityo

AU - Rivaud, Mathilde R.

AU - Marsman, E. Madelief J.

AU - Boender, Arie R.

AU - Klerk, Mischa

AU - Fokkert, Lianne

AU - de Jonge, Berend

AU - Neef, Klaus

AU - Kirzner, Osne F.

AU - Bezzina, Connie R.

AU - Remme, Carol Ann

AU - Tan, Hanno L.

AU - Boukens, Bastiaan J.

AU - Devalla, Harsha D.

AU - Trayanova, Natalia A.

AU - Christoffels, Vincent M.

AU - Barnett, Phil

AU - Boink, Gerard J. J.

PY - 2025/5/7

Y1 - 2025/5/7

N2 - Background and Aims Life-threatening arrhythmias are a well-established consequence of reduced cardiac sodium current (INa). Gene therapy approaches to increase INa have demonstrated potential benefits to prevent arrhythmias. However, the development of such therapies is hampered by the large size of sodium channels. In this study, SCN10A-short (S10s), a short transcript encoding the carboxy-terminal domain of the human neuronal sodium channel, was evaluated as a gene therapy target to increase INa and prevent arrhythmias. Methods Adeno-associated viral vector overexpressing S10s was injected into wild type and Scn5a-haploinsufficient mice on which patch-clamp studies, optical mapping, electrocardiogram analyses, and ischaemia reperfusion were performed.In vitro and in silico studies were conducted to further explore the effect of S10s gene therapy in the context of human hearts. Results Cardiac S10s overexpression increased cellular INa, maximal action potential upstroke velocity, and action potential amplitude in Scn5a-haploinsufficient cardiomyocytes.S10s gene therapy rescues conduction slowing in Scn5a-haploinsufficient mice and prevented ventricular tachycardia induced by ischaemia-reperfusion in wild type mice.S10s overexpression increased maximal action potential upstroke velocity in human inducible pluripotent stem cell-derived cardiomyocytes and prevented inducible arrhythmias in simulated human heart models. Conclusions S10s gene therapy may be effective to treat cardiac conduction abnormalities and associated arrhythmias.

AB - Background and Aims Life-threatening arrhythmias are a well-established consequence of reduced cardiac sodium current (INa). Gene therapy approaches to increase INa have demonstrated potential benefits to prevent arrhythmias. However, the development of such therapies is hampered by the large size of sodium channels. In this study, SCN10A-short (S10s), a short transcript encoding the carboxy-terminal domain of the human neuronal sodium channel, was evaluated as a gene therapy target to increase INa and prevent arrhythmias. Methods Adeno-associated viral vector overexpressing S10s was injected into wild type and Scn5a-haploinsufficient mice on which patch-clamp studies, optical mapping, electrocardiogram analyses, and ischaemia reperfusion were performed.In vitro and in silico studies were conducted to further explore the effect of S10s gene therapy in the context of human hearts. Results Cardiac S10s overexpression increased cellular INa, maximal action potential upstroke velocity, and action potential amplitude in Scn5a-haploinsufficient cardiomyocytes.S10s gene therapy rescues conduction slowing in Scn5a-haploinsufficient mice and prevented ventricular tachycardia induced by ischaemia-reperfusion in wild type mice.S10s overexpression increased maximal action potential upstroke velocity in human inducible pluripotent stem cell-derived cardiomyocytes and prevented inducible arrhythmias in simulated human heart models. Conclusions S10s gene therapy may be effective to treat cardiac conduction abnormalities and associated arrhythmias.

KW - AAV

KW - Cardiac arrhythmia

KW - Gene therapy

KW - SCN10A

KW - SCN5A

KW - Sodium current

UR - https://www.scopus.com/pages/publications/105004775015

U2 - 10.1093/eurheartj/ehaf053

DO - 10.1093/eurheartj/ehaf053

M3 - Article

C2 - 39973098

SN - 0195-668X

VL - 46

SP - 1747

EP - 1762

JO - European heart journal

JF - European heart journal

IS - 18

ER -

SCN10A-short gene therapy to restore conduction and protect against malignant cardiac arrhythmias

Abstract

Keywords

UN SDGs

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