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IA类药物诱发的长QT综合征和尖端扭转型室速患者早期出现类似后除极的活动。

Early afterdepolarizationlike activity in patients with class IA induced long QT syndrome and torsades de pointes.

作者信息

Kurita T, Ohe T, Shimizu W, Suyama K, Aihara N, Takaki H, Kamakura S, Shimomura K

机构信息

Division of Cardiology, National Cardiovascular Center, Osaka, Japan.

出版信息

Pacing Clin Electrophysiol. 1997 Mar;20(3 Pt 1):695-705. doi: 10.1111/j.1540-8159.1997.tb03888.x.

Abstract

Early afterdepolarizations (EADs) have been linked to the mechanism of torsades de pointes in long QT syndrome. The purpose of this study was to investigate the role of EADs in Class IA induced torsades de pointes. We studied nine patients with Class IA induced torsades de pointes at the time this arrhythmia was present (acute period, n = 7) and after Class IA therapy was discontinued (chronic period, n = 6). ECGs and monophasic action potentials were recorded in both periods. In the chronic period, electrophysiological studies were performed before and after disopyramide infusion. In the acute period, QTc interval was markedly prolonged (655 +/- 32 ms1/2), and EAD-like activity was recorded in all patients. QTc interval returned to normal (428 +/- 45 ms1/2) and EAD-like activity disappeared after discontinuation of IA drug. Although, in the chronic period, disopyramide infusion prolonged QTc interval from 428 +/- 48 ms1/2 to 479 +/- 31 ms1/2 and induced EAD in three of six patients, the degree was not as marked as observed in the acute period. EADs may play an important role in the genesis of long QT and torsades de pointes. Disopyramide infusion in the chronic period could not reproduce marked repolarization abnormalities and torsades de pointes.

摘要

早期后除极(EADs)与长QT综合征中尖端扭转型室速的机制有关。本研究的目的是探讨EADs在IA类药物诱发尖端扭转型室速中的作用。我们研究了9例IA类药物诱发尖端扭转型室速的患者,其中7例在心律失常发作时(急性期)进行研究,6例在停用IA类药物治疗后(慢性期)进行研究。在两个时期均记录了心电图和单相动作电位。在慢性期,在静脉输注丙吡胺前后进行了电生理研究。在急性期,QTc间期显著延长(655±32 ms1/2),所有患者均记录到类似EAD的活动。停用IA类药物后,QTc间期恢复正常(428±45 ms1/2),类似EAD的活动消失。虽然在慢性期,静脉输注丙吡胺使QTc间期从428±48 ms1/2延长至479±31 ms1/2,并在6例患者中的3例诱发了EAD,但程度不如急性期明显。EADs可能在长QT和尖端扭转型室速的发生中起重要作用。慢性期静脉输注丙吡胺不能重现明显的复极异常和尖端扭转型室速。

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