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Langendorff心脏模型(Screenit系统)在评估药物致心律失常潜力方面的预测价值综述。

Review of the predictive value of the Langendorff heart model (Screenit system) in assessing the proarrhythmic potential of drugs.

作者信息

Valentin Jean-Pierre, Hoffmann Peter, De Clerck Fred, Hammond Tim G, Hondeghem Luc

机构信息

Safety Assessment UK, AstraZeneca, Mereside Alderley Park, Macclessfield, Cheshire, England, UK.

出版信息

J Pharmacol Toxicol Methods. 2004 May-Jun;49(3):171-81. doi: 10.1016/j.vascn.2004.03.008.

Abstract

Prolongation of the QTc interval of the electrocardiogram (ECG) is used as a surrogate marker for a rare, but life threatening, ventricular arrhythmia known as torsades de pointes (TdP). However, the clear link between QTc prolongation and the arrhythmogenic risk has not been demonstrated unequivocally. In the present review article, we examine (a) the current understanding of electrophysiological and pharmacological mechanisms linking changes in action potential (AP) properties with proarrhythmia and (b) the value of the isolated, paced Langendorff-perfused female rabbit heart model (Screenit system) in predicting the torsadogenic potential of drugs in man. The Screenit system records monophasic action potentials (MAPs) from which the following parameters are evaluated: action potential duration (APD), conduction, instability (indicative of beat to beat APD variability), triangulation (indicative of changes of Phase 3 repolarization), and reverse-use dependency (indicating that the APD is more prolonged at slow heart rates). So far, over 16,000 experiments have been conducted, including approximately 300 dedicated tests to evaluate, in a blinded manner, approximately 70 clinically used drugs. The drugs tested covered a wide range of compounds from various pharmacological and chemical classes with clinical torsadogenic propensity, as well as drugs without the latter effect in clinical settings. Overall, the Screenit system and its associated analysis classified the drugs based on their effects on AP morphology and conduction and additionally identified, in a qualitative manner, drugs clinically associated with TdP. Such an identification is based on the triangulation, reverse-use dependency, and instability of the AP, as well as on the direct indexes of proarrhythmia such as early afterdepolarization (EADs), ventricular tachycardia (VT), and ventricular fibrillation (VF). Overall, drugs that readily induce arrhythmia and/or EADs and/or causes triangulation, reverse-use dependency, and/or instability and/or a chaotic Poincaré plot in a range of concentrations likely to be achieved in man is likely to cause TdP in man, eventually. Only if none of these elements is present, at concentrations well exceeding the free therapeutic plasma concentration, can one expect that the drug will probably be devoid of torsadonenicity. Therefore, this in vitro model provides detailed information on the overall profile of drug-induced electrophysiological effects. In combination with other in vitro and in vivo repolarization assays and with pharmacokinetic data in man, it is a valuable tool to establish an integrated cardiovascular risk assessment of pharmaceutical compounds.

摘要

心电图(ECG)QTc间期延长被用作一种替代标志物,用于指示一种罕见但危及生命的室性心律失常,即尖端扭转型室速(TdP)。然而,QTc延长与心律失常风险之间的明确联系尚未得到明确证实。在本综述文章中,我们研究了:(a)目前对将动作电位(AP)特性变化与促心律失常联系起来的电生理和药理机制的理解;(b)离体、起搏的Langendorff灌注雌性兔心脏模型(Screenit系统)在预测药物对人类的致尖端扭转型室速潜力方面的价值。Screenit系统记录单相动作电位(MAPs),并据此评估以下参数:动作电位时程(APD)、传导、不稳定性(指示逐搏APD变异性)、三角化(指示3期复极化变化)和反向使用依赖性(表明在慢心率时APD延长更明显)。到目前为止,已经进行了超过16000次实验,包括大约300次专门测试,以盲法评估大约70种临床使用的药物。所测试的药物涵盖了来自各种药理和化学类别的广泛化合物,包括具有临床致尖端扭转型室速倾向的化合物,以及在临床环境中无此作用的药物。总体而言,Screenit系统及其相关分析根据药物对AP形态和传导的影响对药物进行分类,并另外定性识别与TdP临床相关的药物。这种识别基于AP的三角化、反向使用依赖性和不稳定性,以及促心律失常的直接指标,如早期后去极化(EADs)、室性心动过速(VT)和室性颤动(VF)。总体而言,在人类可能达到的一系列浓度下,容易诱发心律失常和/或EADs和/或导致三角化、反向使用依赖性和/或不稳定性和/或混乱的庞加莱图的药物最终可能会在人类中引起TdP。只有当这些因素都不存在,且浓度远超过游离治疗血浆浓度时,才可以预期该药物可能没有致尖端扭转型室速的特性。因此,这种体外模型提供了关于药物诱导的电生理效应总体概况的详细信息。与其他体外和体内复极化试验以及人类药代动力学数据相结合,它是建立药物化合物综合心血管风险评估的有价值工具。

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