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Drug Therapy For Torsade de Pointes

机译:尖端扭转型室性心动过速的药物治疗

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Torsade de Pointes. Torsade de pointes is an uncommon and unique type of ventricular tachycardia. It differs from other forms of ventricular tachycardia by its morphological features, underlying mechanism, and modes of therapy. Recognizing torsade de pointes is of major clinical importance, as standard antiarrhythmic regimens might not only be ineffective in abolishing this life‐threatening arrhythmia but may aggravate it. Torsade de pointes is most commonly precipitated by QT prolonging drugs, mainly type IA antiarrhythmic therapy such as quinidine and disopyramide, and other antiarrhythmic agents are reported to cause torsade de pointes as well. Predisposing factors known to increase the likelihood of developing torsade de pointes are: electrolyte imbalance (hypokalemia, hypomagnesemia, or both) and slow heart rate induced either by sinus bradycardia or heart block. Treatment of torsade de pointes is aimed at shortening the QT interval. By acceleration of the heart rate, the QT interval is shortened, thus preventing the recurrence of the arrhythmia. Treatment of torsade de pointes includes: isoproterenol infusion, cardiac pacing, and intravenous atropine. Intravenous magnesium sulfate, a relatively new mode of therapy for torsade de pointes, was proven to be extremely effective and is now regarded as the treatment of choice for this arrhythmia.(Cardiovasc Electrophysiol, Vol. 4, pp. 206–210, April 1
机译:Torsade de Pointes.尖端扭转型室性心动过速是一种罕见且独特的室性心动过速。它与其他形式的室性心动过速的形态学特征、潜在机制和治疗方式不同。识别尖端扭转型室性心动过速具有重要的临床意义,因为标准的抗心律失常方案可能不仅不能有效消除这种危及生命的心律失常,反而可能加重它。尖端扭转型室性心动过速最常由QT间期延长药物诱发,主要是IA型抗心律失常治疗,如奎尼丁和丙吡胺类,据报道其他抗心律失常药物也可引起尖端扭转型室性心动过速。已知增加尖端扭转型室性心动过速可能性的诱发因素包括:电解质失衡(低钾血症、低镁血症或两者兼而有之)和窦性心动过缓或心脏传导阻滞引起的心率减慢。尖端扭转型室性心动过速的治疗旨在缩短QT间期。通过加快心率,缩短QT间期,从而防止心律失常的复发。尖端扭转型室性心动过速的治疗包括:输注异丙肾上腺素、心脏起搏和静脉注射阿托品。静脉注射硫酸镁是一种相对较新的尖端扭转型室性心动过速治疗方式,已被证明非常有效,现在被认为是这种心律失常的首选治疗方法。(Cardiovasc Electrophysiol,第 4 卷,第 206-210 页,4 月 1 日

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