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获得性长QT综合征:利培酮诱发的触发活动及完全性房室传导阻滞时的尖端扭转型室速。I

Acquired long QT syndrome: risperidone-facilitated triggered activity and Torsades de Pointes during complete AV block. I.

作者信息

Raviña Tomas, Raviña Paula, Gutierrez Javier

出版信息

Int J Cardiol. 2007 Apr 4;116(3):416-20. doi: 10.1016/j.ijcard.2006.04.084. Epub 2006 Jul 26.

Abstract

The acquired Long QT Syndrome (aLQTS) is attributed to subtle defects in genes encoding potassium currents (Ik) that may become clinically significant when associated with other factors that impair ventricular repolarization, such as female gender, bradycardia, hypokalemia or the administration of ion channel blocking drugs. We describe full exposure of an aLQTS in a elderly female patient on long-term Risperidone treatment just when bradycardia due to complete AV block developed. We postulate that the aLQTS induced is the result of a combined block of the rapid (I(Kr))and delayed (I(Ks)) components of the Ik current. The electrocardiographic manifestation of (likely) phase 2 early afterdepolarizations and a critical transmural dispersion of repolarization (TDR), both required for the initiation and maintenance of the polymorphic ventricular tachycardia associated with the syndrome (Torsades de Pointes), are as well shown. Risperidone should be used with caution in female patients prone to bradycardia.

摘要

获得性长QT综合征(aLQTS)归因于编码钾电流(Ik)的基因中的细微缺陷,当与其他损害心室复极的因素相关联时,这些缺陷可能具有临床意义,这些因素包括女性性别、心动过缓、低钾血症或使用离子通道阻滞剂。我们描述了一名长期接受利培酮治疗的老年女性患者,在因完全性房室传导阻滞导致心动过缓时,aLQTS完全显现。我们推测,诱发的aLQTS是Ik电流的快速(I(Kr))和延迟(I(Ks))成分联合阻滞的结果。同时还显示了(可能)2期早期后除极的心电图表现以及复极跨壁离散度(TDR)的临界值,这两者都是该综合征相关的多形性室性心动过速(尖端扭转型室速)起始和维持所必需的。对于易发生心动过缓的女性患者,应谨慎使用利培酮。

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