Altered sinoatrial node function and intra-atrial conduction in murine gain-of-function Scn5a +/ΔKPQ hearts suggest an overlap syndrome

Jingjing Wu; Yanmin Zhang; Xinzhao Zhang; Longxian Cheng; Wim J. Lammers; Andrew A. Grace; James A. Fraser; Henggui Zhang; Christopher L.H. Huang; Ming Lei

doi:10.1152/ajpheart.00357.2011

Altered sinoatrial node function and intra-atrial conduction in murine gain-of-function Scn5a ⁺/ΔKPQ hearts suggest an overlap syndrome

Jingjing Wu, Yanmin Zhang, Xinzhao Zhang, Longxian Cheng, Wim J. Lammers, Andrew A. Grace, James A. Fraser, Henggui Zhang, Christopher L.H. Huang, Ming Lei

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

25 Citations (Scopus)

Abstract

Mutations in SCN5A, the gene encoding the pore-forming subunit of cardiac Na ⁺ channels, cause a spectrum of arrhythmic syndromes. Of these, sinoatrial node (SAN) dysfunction occurs in patients with both loss- and gain-of-function SCN5A mutations. We explored for corresponding alterations in SAN function and intracardiac conduction and clarified possible mechanisms underlying these in an established mouse longQTsyndrome type 3 model carrying a mutation equivalent to human SCN5A-ΔKPQ. Electrophysiological characterizations of SAN function in living animals and in vitro sinoatrial preparations were compared with cellular SAN and two-dimensional tissue models exploring the consequences of Scn5a+/ΔKPQ mutations. Scn5a+/ΔKPQ mice showed prolonged electrocardiographic QT and corrected QT intervals confirming long QT phenotypes. They showed frequent episodes of sinus bradycardia, sinus pause/arrest, and significantly longer sinus node recovery times, suggesting compromised pacemaker activity compared with wild-type mice. Electrocardiographic waveforms suggested depressed intra-atrial, atrioventricular node, and intraventricular conduction in Scn5a+/ΔKPQ mice. Isolated Scn5a+/ ΔKPQ sinoatrial preparations similarly showed lower mean intrinsic heart rates and overall slower conduction through the SAN to the surrounding atrium than did wild-type preparations. Computer simulations of both single SAN cells as well as two-dimensional SAN-atrial models could reproduce the experimental observations of impaired pacemaker and sinoatrial conduction in terms of changes produced by both augmented tail and reduced total Na ⁺ currents, respectively. In conclusion, the gain-of-function long QT syndrome type 3 murine Scn5a+/ΔKPQ cardiac system, in overlap with corresponding features reported in loss-of-function Na ⁺ channel mutations, shows compromised SAN pacemaker and conduction function explicable in modeling studies through a combination of augmented tail and reduced peak Na ⁺ currents.

Original language	English
Pages (from-to)	H1510-H1523
Journal	American Journal of Physiology - Heart and Circulatory Physiology
Volume	302
Issue number	7
DOIs	https://doi.org/10.1152/ajpheart.00357.2011
Publication status	Published - Apr 1 2012
Externally published	Yes

Keywords

Long QT syndrome type 3
Sinus node dysfunction
Sodium channel
Type V
Voltage-gated
α-subunit

ASJC Scopus subject areas

Physiology
Cardiology and Cardiovascular Medicine
Physiology (medical)

Access to Document

10.1152/ajpheart.00357.2011

Cite this

Wu, J., Zhang, Y., Zhang, X., Cheng, L., Lammers, W. J., Grace, A. A., Fraser, J. A., Zhang, H., Huang, C. L. H., & Lei, M. (2012). Altered sinoatrial node function and intra-atrial conduction in murine gain-of-function Scn5a ⁺/ΔKPQ hearts suggest an overlap syndrome. American Journal of Physiology - Heart and Circulatory Physiology, 302(7), H1510-H1523. https://doi.org/10.1152/ajpheart.00357.2011

Altered sinoatrial node function and intra-atrial conduction in murine gain-of-function Scn5a ⁺/ΔKPQ hearts suggest an overlap syndrome. / Wu, Jingjing; Zhang, Yanmin; Zhang, Xinzhao et al.
In: American Journal of Physiology - Heart and Circulatory Physiology, Vol. 302, No. 7, 01.04.2012, p. H1510-H1523.

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

Wu, J, Zhang, Y, Zhang, X, Cheng, L, Lammers, WJ, Grace, AA, Fraser, JA, Zhang, H, Huang, CLH & Lei, M 2012, 'Altered sinoatrial node function and intra-atrial conduction in murine gain-of-function Scn5a ⁺/ΔKPQ hearts suggest an overlap syndrome', American Journal of Physiology - Heart and Circulatory Physiology, vol. 302, no. 7, pp. H1510-H1523. https://doi.org/10.1152/ajpheart.00357.2011

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title = "Altered sinoatrial node function and intra-atrial conduction in murine gain-of-function Scn5a +/ΔKPQ hearts suggest an overlap syndrome",

abstract = "Mutations in SCN5A, the gene encoding the pore-forming subunit of cardiac Na + channels, cause a spectrum of arrhythmic syndromes. Of these, sinoatrial node (SAN) dysfunction occurs in patients with both loss- and gain-of-function SCN5A mutations. We explored for corresponding alterations in SAN function and intracardiac conduction and clarified possible mechanisms underlying these in an established mouse longQTsyndrome type 3 model carrying a mutation equivalent to human SCN5A-ΔKPQ. Electrophysiological characterizations of SAN function in living animals and in vitro sinoatrial preparations were compared with cellular SAN and two-dimensional tissue models exploring the consequences of Scn5a+/ΔKPQ mutations. Scn5a+/ΔKPQ mice showed prolonged electrocardiographic QT and corrected QT intervals confirming long QT phenotypes. They showed frequent episodes of sinus bradycardia, sinus pause/arrest, and significantly longer sinus node recovery times, suggesting compromised pacemaker activity compared with wild-type mice. Electrocardiographic waveforms suggested depressed intra-atrial, atrioventricular node, and intraventricular conduction in Scn5a+/ΔKPQ mice. Isolated Scn5a+/ ΔKPQ sinoatrial preparations similarly showed lower mean intrinsic heart rates and overall slower conduction through the SAN to the surrounding atrium than did wild-type preparations. Computer simulations of both single SAN cells as well as two-dimensional SAN-atrial models could reproduce the experimental observations of impaired pacemaker and sinoatrial conduction in terms of changes produced by both augmented tail and reduced total Na + currents, respectively. In conclusion, the gain-of-function long QT syndrome type 3 murine Scn5a+/ΔKPQ cardiac system, in overlap with corresponding features reported in loss-of-function Na + channel mutations, shows compromised SAN pacemaker and conduction function explicable in modeling studies through a combination of augmented tail and reduced peak Na + currents.",

keywords = "Long QT syndrome type 3, Sinus node dysfunction, Sodium channel, Type V, Voltage-gated, α-subunit",

author = "Jingjing Wu and Yanmin Zhang and Xinzhao Zhang and Longxian Cheng and Lammers, {Wim J.} and Grace, {Andrew A.} and Fraser, {James A.} and Henggui Zhang and Huang, {Christopher L.H.} and Ming Lei",

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AU - Cheng, Longxian

AU - Lammers, Wim J.

AU - Grace, Andrew A.

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AB - Mutations in SCN5A, the gene encoding the pore-forming subunit of cardiac Na + channels, cause a spectrum of arrhythmic syndromes. Of these, sinoatrial node (SAN) dysfunction occurs in patients with both loss- and gain-of-function SCN5A mutations. We explored for corresponding alterations in SAN function and intracardiac conduction and clarified possible mechanisms underlying these in an established mouse longQTsyndrome type 3 model carrying a mutation equivalent to human SCN5A-ΔKPQ. Electrophysiological characterizations of SAN function in living animals and in vitro sinoatrial preparations were compared with cellular SAN and two-dimensional tissue models exploring the consequences of Scn5a+/ΔKPQ mutations. Scn5a+/ΔKPQ mice showed prolonged electrocardiographic QT and corrected QT intervals confirming long QT phenotypes. They showed frequent episodes of sinus bradycardia, sinus pause/arrest, and significantly longer sinus node recovery times, suggesting compromised pacemaker activity compared with wild-type mice. Electrocardiographic waveforms suggested depressed intra-atrial, atrioventricular node, and intraventricular conduction in Scn5a+/ΔKPQ mice. Isolated Scn5a+/ ΔKPQ sinoatrial preparations similarly showed lower mean intrinsic heart rates and overall slower conduction through the SAN to the surrounding atrium than did wild-type preparations. Computer simulations of both single SAN cells as well as two-dimensional SAN-atrial models could reproduce the experimental observations of impaired pacemaker and sinoatrial conduction in terms of changes produced by both augmented tail and reduced total Na + currents, respectively. In conclusion, the gain-of-function long QT syndrome type 3 murine Scn5a+/ΔKPQ cardiac system, in overlap with corresponding features reported in loss-of-function Na + channel mutations, shows compromised SAN pacemaker and conduction function explicable in modeling studies through a combination of augmented tail and reduced peak Na + currents.

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