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醋丁洛尔对有显性或隐匿性旁路的患者阵发性房室折返性心动过速的影响。

Effects of acebutolol on paroxysmal atrioventricular reentrant tachycardia in patients with manifest or concealed accessory pathways.

作者信息

Kou H C, Yeh S J, Lin F C, Hung J S, Wu D

出版信息

Chest. 1983 Jan;83(1):92-7. doi: 10.1378/chest.83.1.92.

Abstract

Electrophysiologic studies before and after administration of 50 mg of intravenous (IV) acebutolol were performed in 20 patients. Four of the 20 had persistent preexcitation, two had intermittent preexcitation, and 14 had a concealed retrogradely conducting accessory pathway (AP). Acebutolol depressed anterograde AP conduction with loss of preexcitation in one patient and increased the effective refractory period of AP in the remaining three; in most, it depressed anterograde normal pathway conduction. The longest atrial paced cycle length producing atrioventricular (AV) nodal block increased from 290 +/- 7 to 39 +/- 6 msec (mean +/- SEM) after acebutolol (p less than 0.01). Acebutolol had no significant effect on retrograde AP conduction. Sustained AV reentrant tachycardia was inducible in all 20 patients before acebutolol and in 19 after acebutolol. The cycle length of tachycardia increased from 323 +/- 8 to 352 +/- 8 msec after acebutolol (p less than 0.01), reflecting an increment of A-H interval from 148 +/- 8 to 174 +/- 9 msec (p less than 0.01). Electrophysiologic studies were reported after 800 mg of oral acebutolol given in four divided doses at six-hour intervals in eight patients. The results were comparable to those of IV acebutolol. Thus, acebutolol depresses AV nodal conduction and slows the rate of AV reentrant tachycardia, but is generally ineffective in inhibiting the induction of sustained tachycardia. It occasionally depresses anterograde AP conduction.

摘要

对20例患者在静脉注射50毫克醋丁洛尔前后进行了电生理研究。20例中有4例存在持续性预激,2例有间歇性预激,14例有隐匿性逆向传导旁路(AP)。醋丁洛尔使1例患者的前向AP传导受抑制,预激消失,其余3例AP的有效不应期延长;在大多数患者中,它使前向正常途径传导受抑制。醋丁洛尔应用后,产生房室(AV)结阻滞的最长心房起搏周期长度从290±7毫秒增加到39±6毫秒(均值±标准误)(p<0.01)。醋丁洛尔对逆向AP传导无显著影响。在醋丁洛尔应用前,所有20例患者均可诱发持续性AV折返性心动过速,应用后19例仍可诱发。醋丁洛尔应用后,心动过速的周期长度从323±8毫秒增加到352±8毫秒(p<0.01),反映A-H间期从148±8毫秒增加到174±9毫秒(p<0.01)。对8例患者每隔6小时分4次口服800毫克醋丁洛尔后进行了电生理研究。结果与静脉注射醋丁洛尔的结果相似。因此,醋丁洛尔可抑制AV结传导并减慢AV折返性心动过速的速率,但一般不能有效抑制持续性心动过速的诱发。它偶尔会抑制前向AP传导。

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