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口服磷酸丙吡胺对合并逆向旁道传导的房室折返性心动过速的诱发和维持作用。

Effects of oral disopyramide phosphate on induction and sustenance of atrioventricular reentrant tachycardia incorporating retrograde accessory pathway conduction.

作者信息

Kou H C, Hung J S, Lee Y S, Wu D

出版信息

Circulation. 1982 Aug;66(2):454-62. doi: 10.1161/01.cir.66.2.454.

Abstract

We performed electrophysiologic studies before and after oral administration of disopyramide phosphate, 200 mg every 6 hours, in 20 patients with atrioventricular (AV) reentrant tachycardia using a retrogradely conducting accessory pathway. Disopyramide markedly depressed retrograde accessory pathway conduction by increasing the mean ventricular paced cycle length that produced ventriculoatrial block (less than or equal to 287 +/- 4 to greater than or equal to 392 +/- 22 msec, p less than 0.01); it also depressed antegrade normal pathway AV conduction by increasing the atrial paced cycle length that produced AV block (287 +/- 9 to 328 +/- 7 msec, p less than 0.01). In 14 patients, tachycardia could not be induced or sustained after disopyramide phosphate. In 13 patients, this reflected depression of the retrograde limb with either absence of atrial echoes (nine patients) or induction of nonsustained tachycardia that terminated after the QRS complex (four patients), and in one, it reflected depression of the antegrade limb with induction of a single atrial echo not followed by a QRS response. In six patients, sustained tachycardia could still be induced after disopyramide. Oral disopyramide phosphate is effective in preventing induction of sustained AV reentrant tachycardia in most patients. This effect is achieved by depression of the retrograde limb of the reentrant circuit.

摘要

我们对20例使用逆向传导旁路的房室折返性心动过速患者,在口服磷酸丙吡胺(每6小时200毫克)前后进行了电生理研究。磷酸丙吡胺通过增加产生室房阻滞的平均心室起搏周期长度(从小于或等于287±4毫秒增至大于或等于392±22毫秒,p<0.01),显著抑制逆向旁路传导;它还通过增加产生房室阻滞的心房起搏周期长度(从287±9毫秒增至328±7毫秒,p<0.01),抑制前向正常房室传导。14例患者在服用磷酸丙吡胺后无法诱发或维持心动过速。在13例患者中,这反映了逆向支的抑制,表现为无房回波(9例患者)或诱发非持续性心动过速,在QRS波群后终止(4例患者),在1例患者中,这反映了前向支的抑制,诱发单个房回波但无QRS反应。6例患者在服用磷酸丙吡胺后仍可诱发持续性心动过速。口服磷酸丙吡胺对大多数患者预防持续性房室折返性心动过速的诱发有效。这种作用是通过抑制折返环的逆向支实现的。

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