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α1-肾上腺素受体刺激麻醉兔中导致尖端扭转型室性心动过速的多非利特诱导的生物标志物和内源性决定因素。

Biomarkers and endogenous determinants of dofetilide-induced torsades de pointes in α(1) -adrenoceptor-stimulated, anaesthetized rabbits.

机构信息

2nd Department of Internal Medicine and Cardiology Centre, University of Szeged, Szeged, Hungary.

出版信息

Br J Pharmacol. 2010 Dec;161(7):1477-95. doi: 10.1111/j.1476-5381.2010.00965.x.

Abstract

BACKGROUND AND PURPOSE

Torsades de pointes (TdP) liability is a stochastic event, which indicates that unidentified factors have an important role in facilitating the initiation of TdP by increasing the probability of TdP occurrence. We sought to identify factors that facilitate drug-induced TdP.

EXPERIMENTAL APPROACH

We studied dofetilide-induced TdP in pentobarbital-anaesthetized, phenylephrine-sensitized rabbits, seeking biomarkers that discriminated between the animals that experienced TdP ('TdP+' animals) and those that did not ('TdP-' animals). As novel variables, the beat-to-beat variability and instability of ECG intervals were measured at preset times, irrespective of whether or not hearts were in stable sinus rhythm ('absolute' variability and instability). Autonomic activity was also determined.

KEY RESULTS

Dofetilide delayed repolarization and induced arrhythmias prior to TdP. The variability of the coupling interval and shape of arrhythmic beats before TdP were significantly greater in the 'TdP+' group than in the 'TdP-' group. Accordingly, the 'absolute' variability and instability of the ECG intervals were significantly elevated in the 'TdP+' group. Phenylephrine increased significantly the up-baroreflex sensitivity in the 'TdP+' group before dofetilide administration.

CONCLUSIONS AND IMPLICATIONS

'Preceding' arrhythmias have characteristics that permit prediction of TdP occurrence: the more chaotic the ventricular rhythm, the greater the probability of TdP initiation. This suggests that complexity of the arrhythmic beats may play an important mechanistic role in TdP genesis. The electrical instability quantified by the novel 'absolute' variability and instability parameters correlates with the probability of TdP occurrence. Baroreflex may contribute to TdP genesis in vivo.

摘要

背景与目的

尖端扭转型室性心动过速(TdP)的发生具有随机性,这表明一些未被识别的因素在促进 TdP 的发生中起重要作用,增加了 TdP 的发生概率。我们试图确定促进药物诱导 TdP 的因素。

实验方法

我们在戊巴比妥麻醉、苯肾上腺素敏化的兔中研究了多非利特诱导的 TdP,寻找能够区分经历 TdP(“TdP+”动物)和未经历 TdP(“TdP-”动物)的动物的生物标志物。作为新的变量,我们在预设时间测量心电图(ECG)间期的逐搏变异性和不稳定性,无论心脏是否处于稳定的窦性节律(“绝对”变异性和不稳定性)。同时还测定了自主神经活动。

主要结果

多非利特在 TdP 发生前延迟复极并引起心律失常。在 TdP 之前,“TdP+”组的耦合间期变异性和心律失常搏动的形态明显大于“TdP-”组。因此,“TdP+”组的 ECG 间期“绝对”变异性和不稳定性显著升高。在给予多非利特之前,苯肾上腺素显著增加了“TdP+”组的升压反射敏感性。

结论和意义

“先前”的心律失常具有预测 TdP 发生的特征:室性节律越混乱,发生 TdP 的可能性越大。这表明心律失常的复杂性可能在 TdP 发生机制中起重要作用。通过新的“绝对”变异性和不稳定性参数量化的电不稳定性与 TdP 发生的概率相关。血压反射可能有助于体内 TdP 的发生。

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