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

26 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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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.",

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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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