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在患有慢性房室传导阻滞的犬中,d-索他洛尔和起搏可重复性地诱发早期后除极和尖端扭转型室性心律失常。

Reproducible induction of early afterdepolarizations and torsade de pointes arrhythmias by d-sotalol and pacing in dogs with chronic atrioventricular block.

作者信息

Vos M A, Verduyn S C, Gorgels A P, Lipcsei G C, Wellens H J

机构信息

Department of Cardiology, University Hospital Maastricht, The Netherlands.

出版信息

Circulation. 1995 Feb 1;91(3):864-72. doi: 10.1161/01.cir.91.3.864.

Abstract

It has been well established that antiarrhythmic drugs can also have proarrhythmic effects such as torsade de pointes (TdP) arrhythmias. It was the purpose of this study to create an animal model with a high incidence of reproducible TdP that occurs under clinically relevant circumstances. Experiments were performed in anesthetized dogs that had been in chronic atrioventricular block for 9 +/- 6 weeks. TdP inducibility was attempted using different pacing modes before and after the administration of 2 mg/kg d-sotalol. In some experiments, endocardial monophasic action potentials were recorded. d-Sotalol increased the cycle length of the idioventricular rhythm (1475 +/- 460 to 1730 +/- 570 ms, P < .01) and the QT time (390 +/- 65 to 480 +/- 85 ms, P < .01). In 10% of the experiments, spontaneous TdP occurred after d-sotalol. The incidence of pacing-dependent TdP was 52% (P < .01). In the inducible group, the cycle length of idioventricular rhythm and QT time were significantly longer despite equal percentage increases in these parameters after d-sotalol in both groups. The pacing modes consisting of more than one frequency change had a higher TdP induction rate (P < .05). Reproducibility of TdP induction (three times or more using the same pacing train) remained present for approximately 60 minutes after d-sotalol and was greater than 90% within the same animal over weeks. TdP induction was related to the presence of early afterdepolarizations on the monophasic action potential recordings: five of six in the inducible group versus two of six in the nonresponders. Inducibility could be further increased to 89% when a second bolus of d-sotalol was administered to noninducible dogs. On the other hand, decreasing QT time by faster basic pacing or administration of isoproterenol, or MgSO4 prevented TdP induction. This effect of MgSO4 coincided with the disappearance of early afterdepolarizations. Our animal model shows a high incidence of reproducible acquired TdP arrhythmias, allowing study of the mechanism and treatment of TdP. TdP induction was related to the combination of a slow ventricular rate, the prolongation of QT time, a sudden induced rate change that often required two or more cycle length changes, and the presence of early afterdepolarizations.

摘要

抗心律失常药物也可产生促心律失常作用,如尖端扭转型室性心动过速(TdP),这一点已得到充分证实。本研究的目的是建立一种动物模型,使其在临床相关情况下可重复性发生TdP的发生率较高。实验在慢性房室传导阻滞9±6周的麻醉犬身上进行。在给予2mg/kg d-索他洛尔前后,尝试使用不同的起搏模式诱导TdP。在一些实验中,记录心内膜单相动作电位。d-索他洛尔增加了心室自主节律的周期长度(从1475±460ms增加到1730±570ms,P<.01)和QT间期(从390±65ms增加到480±85ms,P<.01)。在10%的实验中,d-索他洛尔给药后出现自发性TdP。起搏依赖性TdP的发生率为52%(P<.01)。在可诱导组中,尽管两组d-索他洛尔给药后这些参数的增加百分比相同,但心室自主节律的周期长度和QT间期明显更长。由不止一次频率变化组成的起搏模式具有更高的TdP诱导率(P<.05)。d-索他洛尔给药后,TdP诱导的可重复性(使用相同的起搏序列诱导三次或更多次)持续约60分钟,并且在同一动物数周内大于90%。TdP诱导与单相动作电位记录上早期后除极的存在有关:可诱导组6例中有5例,无反应组6例中有2例。当向不可诱导的犬再次推注d-索他洛尔时,诱导率可进一步提高到89%。另一方面,通过更快的基础起搏或给予异丙肾上腺素或硫酸镁来缩短QT间期可预防TdP的诱导。硫酸镁的这种作用与早期后除极的消失同时发生。我们的动物模型显示可重复性获得性TdP心律失常的发生率较高,从而能够对TdP的机制和治疗进行研究。TdP诱导与心室率缓慢、QT间期延长、通常需要两次或更多次周期长度变化的突然诱导率变化以及早期后除极的存在有关。

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