Pulmonary Vein Sleeves as a Pharmacologic Model for the Study of Atrial Fibrillation.

Electrofisiologia & arritmias Pub Date : 2010-10-01
Serge Sicouri, Charles Antzelevitch
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引用次数: 0

Abstract

Objectives: To review the electrophysiologic effects of antiarrhythmic agents in pulmonary veins (PV) sleeve preparations.

Background: Ectopic activity arising from the PV plays a prominent role in the development of atrial fibrillation.

Methods: Transmembrane action potentials were recorded from canine superfused left superior or inferior PV sleeves using standard microelectrode techniques. Acetylcholine (ACh, 1 μM), isoproterenol (1 μM), high calcium ([Ca2+]o=5.4mM) or a combination was used to induce early or delayed afterdepolarizations (EADs or DADs) and triggered activity.

Results: In canine PV sleeves, ranolazine (10 μM) induced a marked use-dependent decrease in Vmax, a rate-dependent abbreviation of action potential duration (APD), but a rate-dependent increase in effective refractory period due to the development of post-repolarization refractoriness and eliminates rate-dependent delayed and late phase 3 early afterdepolarizations (DADs and EADs)-induced triggered activity induced by high calcium, isoproterenol, acetylcholine of their combination together with rapid pacing. Chronic amiodarone induced a prolongation of APD, a marked decrease in Vmax, and prevented the development of DADs and late phase 3 EADs-induced triggered activity. Combination of ranolazine and chronic amiodarone act synergistically to cause potent use-dependent depression of sodium channel-dependent parameters in PV sleeves but not ventricular tissues.

Conclusions: The PV sleeve preparation is a useful model for the study of pharmacologic agents for the treatment of atrial fibrillation. The effectiveness of these agents in arrhythmias induced in PV sleeves may indicate an antiarrhythmic action in eliminating the triggers responsible for AF.

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肺静脉套管作为房颤研究的药理学模型。
目的:探讨抗心律失常药物在肺静脉套筒制剂中的电生理作用。背景:由PV引起的异位活动在房颤的发展中起着重要作用。方法:采用标准微电极技术,记录犬左上、下左PV套筒的跨膜动作电位。乙酰胆碱(ACh, 1 μM),异丙肾上腺素(1 μM),高钙([Ca2+]o=5.4mM)或组合可诱导早期或延迟后去极化(EADs或DADs)并触发活性。结果:在犬PV套管中,芮诺嗪(10 μM)诱导了Vmax的明显使用依赖性降低,动作电位持续时间(APD)的速率依赖性缩短,但有效不应期的速率依赖性增加,这是由于复极化后不应性的发展,并消除了速率依赖性延迟和晚期3期早期去极化(DADs和EADs)诱导的高钙、异丙肾上腺素、乙酰胆碱与它们联合使用,可快速起搏。慢性胺碘酮诱导APD延长,Vmax显著降低,阻止DADs的发展和晚期3期eads诱导的触发活性。雷诺嗪和慢性胺碘酮的联合作用协同作用,导致PV套筒内钠通道依赖性参数的有效使用依赖性抑制,而不是心室组织。结论:PV套筒制备是研究房颤药物治疗的有效模型。这些药物在PV套筒诱发的心律失常中的有效性可能表明其在消除AF触发因素方面具有抗心律失常作用。
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