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钠通道阻滞抗心律失常药物对QRS波晚期电位的选择性延长:与室性心动过速减慢的关系。电生理研究与心电图监测试验(ESVEM)研究者

Selective prolongation of QRS late potentials by sodium channel blocking antiarrhythmic drugs: relation to slowing of ventricular tachycardia. Electrophysiologic Study Versus Electrocardiographic Monitoring Trial (ESVEM) Investigators.

作者信息

Freedman R A, Steinberg J S

机构信息

Department of Internal Medicine, University of Utah School of Medicine, Salt Lake City.

出版信息

J Am Coll Cardiol. 1991 Apr;17(5):1017-25. doi: 10.1016/0735-1097(91)90824-s.

DOI:10.1016/0735-1097(91)90824-s
PMID:1848871
Abstract

Sodium channel blocking antiarrhythmic drugs have preferential effects on diseased, slowly conducting myocardium, and slowing of tachycardia caused by these drugs may result primarily from further prolongation of conduction time in slowly conducting tissue. In patients with sustained ventricular tachycardia, late potentials detected by signal-averaged electrocardiography (ECG) are thought to arise from slowly conducting ventricular myocardium. This study tested the hypothesis that sodium channel blocking drugs selectively prolong the late potential, or terminal low amplitude signal, portion of the signal-averaged QRS complex and that prolongation of the late potential would correlate with slowing of ventricular tachycardia. Fifty-six drug trials in 32 patients with spontaneous and inducible ventricular arrhythmias were studied. Prolongation of the late potential (11 +/- 15 ms) was significantly greater than prolongation of the initial portion of the QRS complex (4 +/- 9 ms) (p = 0.01). Selective prolongation of the late potential by drugs resulted in significantly greater QRS prolongation detectable by signal-averaged ECG than by standard ECG (p less than 0.0001). In 40 trials in which ventricular tachycardia remained inducible during drug therapy, the increase in induced tachycardia cycle length correlated strongly with the increase in late potential duration (p = 0.005) but not with change in the initial portion of the QRS complex. These data suggest that in patients with ventricular tachycardia, sodium channel blocking antiarrhythmic drugs have preferential effects on slowly conducting tissue and that drug effect on slowly conducting tissue contributes to prolongation of ventricular tachycardia cycle length.

摘要

钠通道阻滞型抗心律失常药物对病变的、传导缓慢的心肌具有优先作用,这些药物导致的心动过速减慢可能主要源于缓慢传导组织中传导时间的进一步延长。在持续性室性心动过速患者中,信号平均心电图(ECG)检测到的晚电位被认为源于传导缓慢的心室心肌。本研究检验了以下假设:钠通道阻滞药物选择性延长信号平均QRS波群的晚电位部分,即终末低振幅信号,且晚电位的延长与室性心动过速的减慢相关。对32例伴有自发性和诱发性室性心律失常的患者进行了56次药物试验。晚电位的延长(11±15毫秒)显著大于QRS波群起始部分的延长(4±9毫秒)(p = 0.01)。药物对晚电位的选择性延长导致信号平均心电图检测到的QRS延长显著大于标准心电图(p<0.0001)。在40次药物治疗期间室性心动过速仍可诱发的试验中,诱发的心动过速周期长度的增加与晚电位持续时间的增加密切相关(p = 0.005),但与QRS波群起始部分的变化无关。这些数据表明,在室性心动过速患者中,钠通道阻滞型抗心律失常药物对缓慢传导组织具有优先作用,且药物对缓慢传导组织的作用有助于延长室性心动过速的周期长度。

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