Antiarrhythmic effect of a new class 1 antiarrhythmic drug, AN-132, on ventricular arrhythmias in beagles

Hashimoto, Keitaro; Watanabe, Kozo; Mitsuhashi, Harumi

doi:10.1007/bf01857620

Cited by 5 publications

(7 citation statements)

References 7 publications

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“…Although these arrhythmias most likely are caused by triggered activity from delayed after depolarizations, ab normal automaticity and/or re-entrant excitation in very depolarized tissues (11,39,40), a good correlation was found only between EDSO(IVCT) in this current study and IC50 of two different types of arrhythmia models. The results may indicate that the antiarrhythmic mechanism of class I drugs in the canine arrhythmia models is closely related to the suppression of the normal intraventricular conduction.…”

Section: Discussionmentioning

confidence: 42%

“…Other drugs were tested at 500-msec driving interval. An tiarrhythmic plasma concentrations were calculated from our earlier reports (11,39,40). P: procainamide, D: disopyramide, L4: lido caine at 400-msec driving interval, L3: lidocaine at 300-msec driving interval, M4: mexiletine at 400-msec driving interval, M3: mexiletine at 300-msec driving interval, F: flecainide, ME: ME3202, AN: AN 132.…”

Section: Discussionmentioning

confidence: 99%

“…Correlation between cardiac direct effects and antiar rhythmic activity: We examined the correlation between the intraarterial ED50 doses in this study and the antiar rhythmic IC50 plasma concentrations obtained in our previous canine arrhythmia model studies, namely digi talis and coronary ligation-induced arrhythmias (11,39,40). Although these arrhythmias most likely are caused by triggered activity from delayed after depolarizations, ab normal automaticity and/or re-entrant excitation in very depolarized tissues (11,39,40), a good correlation was found only between EDSO(IVCT) in this current study and IC50 of two different types of arrhythmia models.…”

Section: Discussionmentioning

confidence: 99%

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Utilization of an Isolated, Blood-Perfused Canine Papillary Muscle Preparation as a Model to Assess Efficacy and Adversity of Class I Antiarrhythmic Drugs

Sugiyama

Motomura

Hashimoto

1994

Japanese Journal of Pharmacology

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ABSTRACT-To develop a model to predict the efficacy and adversity of class I antiarrhythmic drugs, intra ventricular conduction time (IVCT), coronary blood flow (CBF), developed tension of papillary muscle (DT) and idioventricular automaticity rate (VR) were measured following drug administration in an isolated canine papillary muscle preparation cross-circulated with the heparinized blood of a donor dog. Tetrodo toxin, the prototypic fast Na+ channel blocker, and class I drugs increased IVCT and CBF, but decreased DT and VR, in a dose-dependent manner. The profiles of known class I drugs, procainamide, disopyramide, lidocaine, mexiletine and flecainide were similar, but the potencies of each drug were different. Two new class I drugs, ME3202 and AN-132, were also tested and found to have effects that were similar to that of tetrodotoxin. There was a good correlation between the doses of drugs prolonging IVCT by 50010 and the canine antiarrhythmic plasma concentrations in our previous study. This model can also be used to estimate the use-dependency and the kinetics of use-dependent sodium channel block; however, it is not suitable for extensive investigation of cellular and molecular mechanisms. Thus, the use of this model facilitates the com parison of multiple cardiac effects of class I drugs and may be an effective way to better assess new antiar rhythmic drugs.

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Section: Discussionmentioning

confidence: 42%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Utilization of an Isolated, Blood-Perfused Canine Papillary Muscle Preparation as a Model to Assess Efficacy and Adversity of Class I Antiarrhythmic Drugs

Sugiyama

Motomura

Hashimoto

1994

Japanese Journal of Pharmacology

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“…As reported earlier [1,2,[5][6][7][8][9][11][12][13][14][15][16][17][18]20,21,[23][24][25][26][27][28][29][30][31][32], mongrel and beagle dogs of either sex, as well as female beagle dogs, weighing about 7-15 kg, were anesthetized initially with thiopental sodium. After intubation, 1.0% halothane, vaporized with 100% oxygen, was administered with a volume-limited ventilator (20 ml/kg, 15 strokes/min).…”

Section: Production Of Adrenaline-induced Arrhythmiamentioning

confidence: 99%

“…For intravenous infusion studies, a constant-rate infusion was performed for 10 minutes using a syringe pump, and arterial blood samples were drawn from one lumen of the arterial double-lumen cannula at 0, 1, 3,5,7,9,13,15,30, and 60 minutes after the start of the infusion. [6][7][8]12,14,17,18,[20][21][22][23][24][25][26][27][28][29][30][31][32], female beagle dogs, weighing about 7-12 kg, were anesthetized initially with intravenous thiopental sodium, 30 mg/kg, and intubated. The chest was opened and a two-stage coronary ligation of the left anterior descending artery (LAD) was performed under halothane anesthesia.…”

mentioning

confidence: 99%

Effects of antiarrhythmic drugs on canine ventricular arrhythmia models: Which electrophysiological characteristics of drugs are related to their effectiveness?

Hashimoto

Haruno

Matsuzaki

et al. 1991

Cardiovasc Drug Ther

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In order to compare and clarify the effects of various antiarrhythmic drugs when given as monotherapy, we reevaluated our previous data on antiarrhythmic drugs and recalculated antiarrhythmic plasma concentrations of drugs for several canine arrhythmia models. We used three spontaneously occurring arrhythmias: a) digitalis-, b) two-stage coronary ligation-, and c) adrenaline-induced arrhythmias. All antiarrhythmic drugs of class I suppressed digitalis arrhythmia, and, except for lidocaine, also suppressed coronary ligation arrhythmia. Class II antiarrhythmic drugs, beta blockers, and class IV antiarrhythmic drugs, Ca antagonists, had common features of effectiveness and suppressed adrenaline arrhythmia in relatively low concentrations. Class III drugs were not effective on these three arrhythmias. Differences among the antiarrhythmic effects of class I drugs could not be explained by their subclassification based either on action potential duration or kinetic properties of dissociation or association with Na channels. New triggered arrhythmia models in vivo and in vitro canine hearts were developed, and drug effects were not the same as those on the three spontaneously occurring arrhythmia models.

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Effects of SEA0400, a Na+/Ca2+ exchange inhibitor, on ventricular arrhythmias in the in vivo dogs

Nagasawa

Zhu

Chen

et al. 2005

European Journal of Pharmacology

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Antiarrhythmic effect of a new class 1 antiarrhythmic drug, AN-132, on ventricular arrhythmias in beagles

Cited by 5 publications

References 7 publications

Utilization of an Isolated, Blood-Perfused Canine Papillary Muscle Preparation as a Model to Assess Efficacy and Adversity of Class I Antiarrhythmic Drugs

Utilization of an Isolated, Blood-Perfused Canine Papillary Muscle Preparation as a Model to Assess Efficacy and Adversity of Class I Antiarrhythmic Drugs

Effects of antiarrhythmic drugs on canine ventricular arrhythmia models: Which electrophysiological characteristics of drugs are related to their effectiveness?

Effects of SEA0400, a Na+/Ca2+ exchange inhibitor, on ventricular arrhythmias in the in vivo dogs

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