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尖端扭转型室性心动过速:预防与治疗

Torsades de pointes: prevention and therapy.

作者信息

Keren A, Tzivoni D

机构信息

Heiden Department of Cardiology, Bikur Cholim Hospital, Jerusalem, Israel.

出版信息

Cardiovasc Drugs Ther. 1991 Apr;5(2):509-13. doi: 10.1007/BF03029778.

Abstract

Torsades de pointes (TdP) is a life-threatening ventricular tachycardia that occurs in the setting of a prolonged QT interval and is most frequently related to administration of antiarrhythmic drugs. Patients with organic heart disease, with low serum electrolyte levels, with a previous episode of TdP and with bradycardia or baseline QT prolongation may be at increased risk of developing TdP. After initiation of a QT prolonging therapy, the dosage should be modified if the QT interval reaches 560-600 ms. Cessation of medication and immediate hospitalization are indicated in the presence of lightheadedness, syncope, or increased frequency and complexity of ventricular premature beats. The conventional therapy of TdP with isoproterenol or cardiac pacing, although usually effective, has certain disadvantages. Isoproterenol is contraindicated in patients with hypertension or ischemic heart disease, whereas institution of cardiac pacing requires skilled personnel and fluoroscopy. Recently, infusion of magnesium sulfate has been shown to abolish TdP both in the clinical and experimental setting. Compared with conventional therapy, magnesium sulfate has the advantage of safety and simplicity of its administration. In doubtful cases, if does not aggravate a ventricular tachycardia that is not TdP, as may occur with isoproterenol. This advantage and the prompt effectiveness of the drug in four clinical series, including 31 patients, support the use of magnesium sulfate as the first line of therapy for TdP.

摘要

尖端扭转型室性心动过速(TdP)是一种危及生命的室性心动过速,发生于QT间期延长的情况下,最常与抗心律失常药物的使用有关。患有器质性心脏病、血清电解质水平低、既往有TdP发作史以及心动过缓或基线QT延长的患者发生TdP的风险可能增加。开始使用延长QT间期的治疗后,如果QT间期达到560 - 600毫秒,应调整剂量。出现头晕、晕厥或室性早搏频率和复杂性增加时,应停药并立即住院。用异丙肾上腺素或心脏起搏对TdP进行传统治疗,虽然通常有效,但有一定缺点。异丙肾上腺素在高血压或缺血性心脏病患者中禁用,而进行心脏起搏需要技术熟练的人员和荧光透视检查。最近,硫酸镁静脉输注已被证明在临床和实验环境中都能消除TdP。与传统治疗相比,硫酸镁具有安全性高和给药简单的优点。在可疑病例中,如果不加重非TdP的室性心动过速(异丙肾上腺素可能会加重)。这种优点以及该药物在包括31例患者的四个临床系列中的迅速有效性,支持将硫酸镁作为TdP的一线治疗药物。

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