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Literature DB >> 19351517

Arrhythmogenic substrate and its modification by nicorandil in a murine model of long QT type 3 syndrome.

Sandeep S Hothi¹, Stephen W Booth, Ian N Sabir, Matthew J Killeen, Fergus Simpson, Yanmin Zhang, Andrew A Grace, Christopher L-H Huang.

Abstract

The gain-of-function Scn5a+/DeltaKPQ mutation in the cardiac Na(+) channel causes human long QT type 3 syndrome (LQT3) associated with ventricular arrhythmogenesis. The K(ATP) channel-opener nicorandil (20muM) significantly reduced arrhythmic incidence in Langendorff-perfused Scn5a+/Delta hearts during programmed electrical stimulation; wild-types (WTs) showed a total absence of arrhythmogenicity. These observations precisely correlated with alterations in recently established criteria for re-entrant excitation reflected in: (1) shortened left-ventricular epicardial but not endocardial monophasic action potential durations at 90% repolarization (APD(90)) that (2) restored transmural repolarization gradients, DeltaAPD(90). Scn5a+/Delta hearts showed longer epicardial but not endocardial APD(90)s, giving shorter DeltaAPD(90)s than WT hearts. Nicorandil reduced epicardial APD(90) in both Scn5a+/Delta and WT hearts thereby increasing DeltaAPD(90). (3) Reduced epicardial critical intervals for re-excitation; Scn5a+/Delta hearts showed greater differences between APD(90) and ventricular effective refractory period than WT hearts that were reduced by nicorandil. (4) Reduced APD(90) alternans. Scn5a+/Delta hearts showed greater epicardial and endocardial alternans than WTs, which increased with pacing rate. Nicorandil reduced these in Scn5a+/Delta hearts to levels indistinguishable from untreated WTs. (5) Flattened restitution curves. Scn5a+/Delta hearts showed larger epicardial and endocardial critical diastolic intervals than WT hearts. Nicorandil decreased these in Scn5a+/Delta and WT hearts. The presence or absence of arrhythmogenesis in Scn5a+/Delta and WT hearts thus agreed with previously established criteria for re-entrant excitation, and alterations in these precisely correlated with the corresponding antiarrhythmic effects of nicorandil. Together these findings implicate spatial and temporal re-entrant mechanisms in arrhythmogenesis in LQT3 and their reversal by nicorandil.

Entities: Chemical Disease Gene Species

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Year: 2009 PMID： 19351517 DOI： 10.1016/j.pbiomolbio.2009.01.006

Source DB: PubMed Journal: Prog Biophys Mol Biol ISSN： 0079-6107 Impact factor: 3.667

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Cited

8 in total

1. Ventricular arrhythmogenesis following slowed conduction in heptanol-treated, Langendorff-perfused mouse hearts.

Authors: Gary Tse; Sandeep S Hothi; Andrew A Grace; Christopher L-H Huang
Journal: J Physiol Sci Date: 2012-01-05 Impact factor: 2.781

2. Autonomic modulation and antiarrhythmic therapy in a model of long QT syndrome type 3.

Authors: Larissa Fabritz; Dierk Damke; Markus Emmerich; Susann G Kaufmann; Kathrin Theis; Andreas Blana; Lisa Fortmüller; Sandra Laakmann; Sven Hermann; Elena Aleynichenko; Johannes Steinfurt; Daniela Volkery; Burkhard Riemann; Uwe Kirchhefer; Michael R Franz; Günter Breithardt; Edward Carmeliet; Michael Schäfers; Sebastian K G Maier; Peter Carmeliet; Paulus Kirchhof
Journal: Cardiovasc Res Date: 2010-01-28 Impact factor: 10.787

3. Empirical correlation of triggered activity and spatial and temporal re-entrant substrates with arrhythmogenicity in a murine model for Jervell and Lange-Nielsen syndrome.

Authors: Sandeep S Hothi; Glyn Thomas; Matthew J Killeen; Andrew A Grace; Christopher L-H Huang
Journal: Pflugers Arch Date: 2009-05-09 Impact factor: 3.657

Arrhythmogenic substrate and its modification by nicorandil in a murine model of long QT type 3 syndrome.

1. Ventricular arrhythmogenesis following slowed conduction in heptanol-treated, Langendorff-perfused mouse hearts.

2. Autonomic modulation and antiarrhythmic therapy in a model of long QT syndrome type 3.

3. Empirical correlation of triggered activity and spatial and temporal re-entrant substrates with arrhythmogenicity in a murine model for Jervell and Lange-Nielsen syndrome.

Review 4. Murine Electrophysiological Models of Cardiac Arrhythmogenesis.

5. Mouse Models of SCN5A-Related Cardiac Arrhythmias.

Review 6. Ion channels, long QT syndrome and arrhythmogenesis in ageing.

7. Cardiac electrophysiological adaptations in the equine athlete-Restitution analysis of electrocardiographic features.

8. Determination of action potential wavelength restitution in Scn5a^+/- mouse hearts modelling human Brugada syndrome.

Arrhythmogenic substrate and its modification by nicorandil in a murine model of long QT type 3 syndrome.

1. Ventricular arrhythmogenesis following slowed conduction in heptanol-treated, Langendorff-perfused mouse hearts.

2. Autonomic modulation and antiarrhythmic therapy in a model of long QT syndrome type 3.

3. Empirical correlation of triggered activity and spatial and temporal re-entrant substrates with arrhythmogenicity in a murine model for Jervell and Lange-Nielsen syndrome.

Review 4. Murine Electrophysiological Models of Cardiac Arrhythmogenesis.

5. Mouse Models of SCN5A-Related Cardiac Arrhythmias.

Review 6. Ion channels, long QT syndrome and arrhythmogenesis in ageing.

7. Cardiac electrophysiological adaptations in the equine athlete-Restitution analysis of electrocardiographic features.

8. Determination of action potential wavelength restitution in Scn5a+/- mouse hearts modelling human Brugada syndrome.

8. Determination of action potential wavelength restitution in Scn5a^+/- mouse hearts modelling human Brugada syndrome.