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决奈达隆诱导的心室复极变化的动态分析。

Dynamic analysis of dofetilide-induced changes in ventricular repolarization.

作者信息

Lande G, Maison-Blanche P, Fayn J, Ghadanfar M, Coumel P, Funck-Brentano C

机构信息

Department of Cardiology, Lariboisière Hospital, Paris, France.

出版信息

Clin Pharmacol Ther. 1998 Sep;64(3):312-21. doi: 10.1016/S0009-9236(98)90180-1.

Abstract

OBJECTIVE

To use dynamic electrocardiographic (ECG) techniques to study the influence of heart rate on dofetilide-induced QT prolongation among healthy volunteers.

BACKGROUND

The extent to which heart rate modulates QT prolongation induced by the new class III antiarrhythmic drug dofetilide is a matter of debate.

METHODS

Ten healthy volunteers underwent two 24-hour ECG recordings, one in the absence of dofetilide and the other after a single oral dose of 0.5 mg dofetilide. Two 4-hour periods were defined during the second recording: Dh, which corresponded to stable high concentration of the drug, and D1, which corresponded to low concentration of the drug. Corresponding baseline recording periods, Ch and C1, matched by time with Dh and D1 were selected from the control ECG recording in the absence of dofetilide. QT versus R-R relations were compared in the presence and absence of dofetilide. The QT versus R-R relation slope was used as an index of the rate dependence QT prolongation. Rate-independent changes in QT duration were also analyzed.

RESULTS

During Dh, dofetilide induced a mean 12% lengthening of ventricular repolarization. Dynamic ECG analysis showed that this prolongation increased as R-R cycles became longer, a phenomenon known as reverse rate dependence. However, QT prolongation persisted at the shortest (600 ms) R-R cycle length that could be analyzed. During D1, dynamic ECG analysis showed a persistent, although small, effect of dofetilide on both QT prolongation (3%) and reverse rate dependence of this effect.

CONCLUSIONS

Dofetilide prolongs QT duration, and this class III effect is influenced by heart rate. Although dofetilide-induced QT prolongation decreases when the R-R cycle shortens, this reverse rate dependence is only partial because marked QT prolongation persists at an R-R cycle of 600 ms. The results of our study indicated that dynamic ECG techniques can be useful in detection of subtle, drug-induced changes in the duration of ventricular repolarization.

摘要

目的

运用动态心电图(ECG)技术研究心率对健康志愿者中多非利特所致QT间期延长的影响。

背景

心率对新型III类抗心律失常药物多非利特所致QT间期延长的调节程度存在争议。

方法

10名健康志愿者接受了两次24小时心电图记录,一次在未服用多非利特时进行,另一次在口服0.5mg多非利特单次剂量后进行。在第二次记录期间定义了两个4小时时段:Dh,对应药物稳定高浓度;D1,对应药物低浓度。从未服用多非利特的对照心电图记录中选取与Dh和D1时间匹配的相应基线记录时段Ch和C1。比较有无多非利特时QT与R-R关系。QT与R-R关系斜率用作心率依赖性QT间期延长的指标。还分析了QT间期的非心率依赖性变化。

结果

在Dh期间,多非利特使心室复极平均延长12%。动态心电图分析显示,随着R-R周期变长,这种延长增加,这一现象称为反向心率依赖性。然而,在可分析的最短(600毫秒)R-R周期长度时,QT间期延长仍然存在。在D1期间,动态心电图分析显示多非利特对QT间期延长(3%)及其反向心率依赖性均有持续但较小的影响。

结论

多非利特可延长QT间期,且这种III类效应受心率影响。尽管当R-R周期缩短时多非利特所致的QT间期延长会减少,但这种反向心率依赖性只是部分存在,因为在600毫秒的R-R周期时仍有明显的QT间期延长。我们的研究结果表明,动态心电图技术可用于检测心室复极时长细微的药物诱导变化。

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