Decrease of epinephrine-induced arrhythmia threshold in ethanol exposed rats

Hoffmann, Peter; Müller, S; Zbinden, G.

doi:10.1007/bf02035134

Cited by 2 publications

(1 citation statement)

References 14 publications

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“…Tripathi et al (13) produced ventricular tachycardia by a bolus infusion of adrenaline at a dose 10 m g / kg intravenously in the rat and guinea pig anesthetized with intraperitoneal injection of urethane. Hoffman et al (14) investigated the effects of ethanol treatment on adrenaline-induced arrhythmias in rats. They infused adrenaline at a rate of 10 mg/ kg per min intravenously.…”

Section: Arrhythmogenic Dose Of Adrenalinementioning

confidence: 99%

Development of a Halothane-Adrenaline Arrhythmia Model Using In Vivo Guinea Pigs

Noda

Hashimoto

2004

J Pharmacol Sci

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Abstract. In vivo antiarrhythmic effects of diltiazem hydrochloride and nifekalant hydrochloride, a pure class III antiarrhythmic drug (Vaughan Williams' classification), on adrenaline induced ventricular arrhythmias were examined in halothane anesthetized guinea pigs. Continuous adrenaline infusion (12.5 m g / kg per min) induced ventricular arrhythmias. Arrhythmogenicity was significantly increased with vagotomy and higher concentration of halothane. After injection of diltiazem at 0.5 mg / kg, the arrhythmic ratio (the number of ventricular ectopic beats divided by the total heart beats) was significantly reduced compared with the predrug control value (0.69 vs 0.04, P<0.05). No significant change of arrhythmic ratio was observed after injection of nifekalant (0.57 vs 0.61, ns). After administration of nifekalant, the mean minimum adrenaline infusion rate that induced ventricular arrhythmia decreased from 9.29 to 6.43 m g / kg per min. On the other hand, before administration of diltiazem, the mean arrhythmogenic rate of adrenaline was 8.50 mg / kg per min, but ventricular arrhythmias were no longer induced during continuous infusion of diltiazem at 0.5 mg / kg per min. These results were qualitatively consistent with previous experiments using the canine halothane-adrenaline model. In conclusion, the halothaneadrenaline arrhythmia model using the in vivo guinea pig is useful for screening drugs with potential anti-or pro-arrhythmic properties.

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Section: Arrhythmogenic Dose Of Adrenalinementioning

confidence: 99%

Development of a Halothane-Adrenaline Arrhythmia Model Using In Vivo Guinea Pigs

Noda

Hashimoto

2004

J Pharmacol Sci

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Barium Chloride-Induced Cardiac Arrhythmia Mouse Model Exerts an Experimental Arrhythmia for Pharmacological Investigations

Zeng,

Huang,

Zheng

et al. 2024

Life

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Aim: Cardiac arrhythmias are among the most important pathologies that cause sudden death. The exploration of new therapeutic options against arrhythmias with low undesirable effects is of paramount importance. Methods: However, the convenient and typical animal model for screening the potential lead compound becomes a very critical modality, particularly in anti-arrhythmia. In this study, mice were intraperitoneally (i.p.) injected with BaCl2, CaCl2, and adrenaline to induce arrhythmia, and simultaneously compared with BaCl2-induced rats. Results: Electrocardiogram (ECG) showed that the majority of mice repeatedly developed ventricular bigeminy, ventricular tachycardia (VT), and ventricular fibrillation (VF) after BaCl2-injection as seen in rats. The ECG of mice developed ventricular bigeminy and VT after CaCl2 and AT after adrenaline i.p. injection. Additionally, acute cardiac arrhythmia after BaCl2 i.p. injection could be reverted by drugs (lidocaine and amiodarone) administration. Additionally, the different routes of administration for various chemical-induced arrhythmia in both mice and rats were also retrieved from PubMed and summarized. Comparing this approach with previous studies after the literature review reveals that arrhythmia of BaCl2-induced i.p. mice is compatible with the induction of other routes. Conclusions: This study brings an alternative experimental model to investigate antiarrhythmic theories and provides a promising approach to discovering new interventions for acute arrhythmias.

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Decrease of epinephrine-induced arrhythmia threshold in ethanol exposed rats

Cited by 2 publications

References 14 publications

Development of a Halothane-Adrenaline Arrhythmia Model Using In Vivo Guinea Pigs

Development of a Halothane-Adrenaline Arrhythmia Model Using In Vivo Guinea Pigs

Barium Chloride-Induced Cardiac Arrhythmia Mouse Model Exerts an Experimental Arrhythmia for Pharmacological Investigations

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