南方医科大学学报

南方医科大学学报 ›› 2013, Vol. 33 ›› Issue (07): 1093-.

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药物致尖端扭转型室性心动过速的发生机制

王军奎,于忠祥,崔长琮   

  • 出版日期:2013-07-20 发布日期:2013-07-20

Mechanism of drug-induced torsade de pointes: an experimental study in dogs

  • Online:2013-07-20 Published:2013-07-20

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摘要: 目的探讨药物致尖端扭转型室性心动过速(Tdp)的发生机制。方法建立冠状动脉灌注的犬左室心肌楔形组织块模型,
同步记录左心室内膜、中层、外膜心肌细胞的动作电位及跨壁心电图,观察不同浓度D-Sotalol对动作电位时间(APD)、QT间期、
跨壁复极离散度(TDR)、早期后除极(EAD)及Tdp发生的影响。结果浓度为0~100 μmol/L的D-Sotalol呈剂量依赖性地延长
各层细胞APD,尤以中层细胞最为显著(P<0.05),因而增加TDR;D-Sotalol在中层细胞可诱发EAD,触发室性早博并形成跨壁
折返导致Tdp。结论D-Sotalol在中层细胞诱发EAD、R on T室性早博是其致Tdp的始动因子,在TDR增加的基础上形成跨室
壁折返是Tdp得以维持的关键。

Abstract: Objective To investigate the mechanism of drug-induced torsade de pointes (Tdp) in dogs. Methods In arterially
perfused canine left ventricular wedge preparations, the action potential duration (APD) of the endocardial (Endo),
midomyocardial (M) and epicardial (Epi) myocytes, and transmural electrocardiogram (ECG) were recorded simultaneously.
The effects of different concentrations of D-Sotalol on APD, transmural dispersion of repolarization (TDR), early
afterdepolarization (EAD) and Tdp were observed. Results D-Sotalol prolonged APD of the Endo, M and Epi cells in a
concentration-dependent manner from 0-100 μmol/L, and increased TDR due to a preferential APD prolongation of the M cells
relative to Epi and Endo cells. The application of D-Sotalol elicited EAD, R on T ventricular premature beats, transmural
reentry and Tdp in the M cells. Conclusion EAD and R on T ventricular premature beats induced by D-Sotalol in M cells
triggers Tdp, which is maintained by TDR increment and transmural reentry.