Programmed ventricular stimulation after myocardial infarction does not help reduce the risk of ventricular events

Brembilla‐Perrot, Béatrice; Jacquemin, L.; A, Terrier de la Chaise; Beurrier, Daniel

doi:10.1007/bf00050995

Cardiovasc Drug Ther

1996

DOI: 10.1007/bf00050995

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Programmed ventricular stimulation after myocardial infarction does not help reduce the risk of ventricular events

Béatrice Brembilla‐Perrot¹,

L. Jacquemin²,

Terrier de la Chaise A³

et al.

Abstract: Programmed ventricular stimulation could be a useful technique to detect patients at high risk for ventricular arrhythmias and sudden death after acute myocardial infarction. However, prevention of arrhythmic events using this technique has never been demonstrated. To determine whether prophylactic antiarrhythmic therapy influences prognosis after acute myocardial infarction, 196 patients without spontaneous ventricular tachycardia (VT) but with inducible sustained monomorphic VT were followed for 3 +/- 1 year… Show more

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Cited by 4 publications

References 25 publications

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Arrhythmogenic potential of positive inotropic agents

Stump¹,

Wallace²,

Gilberto³

et al. 2000

Basic Research in Cardiology

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The clinical use of positive inotropic agents has been associated with increased mortality, with proarrhythmia speculated to be a contributing factor. This study compares the arrhythmogenic potentials of six positive inotropic agents representing different mechanistic classes: the beta-adrenergic agonist dobutamine, the adenylyl cyclase activator forskolin, the phosphodiesterase-III inhibitor milrinone, the cardiac glycoside ouabain, and the sodium channel agonists DPI 201-106 and BDF 9148. These agents were studied in dogs with anterior myocardial infarction using lower and higher dose i.v. regimens targeted to elicit 20-40% and 70-90% increases in LV+dP/dt, respectively. Precipitation of new ventricular arrhythmia by programmed ventricular stimulation was observed in all treatment groups. Incidences of new arrhythmia were comparable in the lower dose regimens, ranging from 16.7% (3/18 animals with BDF 9148) to 31.6% (6/19 animals with DPI 201-106), and in the higher dose regimens, ranging from 10.0% (1/10 animals with milrinone) to 27.7% (5/18 animals with DPI 201-106). The overall incidence of new ventricular arrhythmia ranged from 27.3% (3/11 animals with ouabain) to 47.4% (9/19 animals with DPI 201-106). No differences were observed in underlying infarct size or time from infarction to electrophysiologic study between subgroups of animals in which new arrhythmias were precipitated vs. those remaining non-responsive in any treatment group. The positive inotropic agents tested displayed diverse total group effects on heart rate, electrocardiographic intervals including QTc and ventricular refractoriness. Within individual treatment comparisons revealed a general but not universal pattern of greater ventricular refractory period values in newly inducible vs. non-inducible subgroups in the DPI 201-106, BDF 9148 and ouabain (low and high dose); milrinone and dobutamine (high dose) treatment groups. These findings indicate that regardless of underlying cellular mechanism of action, the six positive inotropic agents tested all displayed comparable proarrhythmic potentials unrelated to underlying infarct size and time from infarction. This observation suggests the general shared property of increased myocardial contractility, potentially adversely affecting myocardial oxygen balance, myocardial perfusion and electrical stability in the setting of previous myocardial infarction, to be a common underlying cause for arrhythmogenesis. Additionally, alterations in ventricular refractoriness and repolarization may contribute significantly to proarrhythmia with some positive inotropic interventions.

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Arrhythmogenic potential of positive inotropic agents

Stump¹,

Wallace²,

Gilberto³

et al. 2000

Basic Research in Cardiology

View full text Add to dashboard Cite

show abstract

La syncope change-t-elle les résultats de la stimulation ventriculaire programmée chez les patients ayant un antécédent d’infarctus du myocarde ?

Brembilla‐Perrot

Suty-Selton

Beurrier

et al. 2004

Annales de Cardiologie et d'Angéiologie

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Une étude électrophysiologique complète reste nécessaire dans une cardiopathie évoluée symptomatique

Brembilla-Perrot¹,

Claudon²,

Marçon³

et al. 2010

Annales de Cardiologie et d'Angéiologie

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Programmed ventricular stimulation after myocardial infarction does not help reduce the risk of ventricular events

Cited by 4 publications

References 25 publications

Arrhythmogenic potential of positive inotropic agents

Arrhythmogenic potential of positive inotropic agents

La syncope change-t-elle les résultats de la stimulation ventriculaire programmée chez les patients ayant un antécédent d’infarctus du myocarde ?

Une étude électrophysiologique complète reste nécessaire dans une cardiopathie évoluée symptomatique

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