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氟司洛尔治疗无相关结构性心脏病的室上性心动过速的电药理学研究

Electropharmacology of flestolol for supraventricular tachycardia without associated structural heart disease.

作者信息

Swerdlow C, Peterson J, Liem L B, Blake K, Franz M R, Laddu A

机构信息

Cardiology Division, Stanford University Medical Center, California 94305.

出版信息

Am J Cardiol. 1987 Nov 1;60(13):1055-60. doi: 10.1016/0002-9149(87)90351-1.

DOI:10.1016/0002-9149(87)90351-1
PMID:2890290
Abstract

Flestolol is an ultrashort-acting beta-blocking drug with a half-life of 6.9 minutes. Its antiarrhythmic efficacy was studied in 21 patients with spontaneous and inducible supraventricular tachycardia: atrioventricular (AV) nodal tachycardia in 6 patients and orthodromic AV reciprocating tachycardia in 15. It increased the effective refractory period of the AV node in all patients with AV nodal tachycardia (fast pathway, p less than 0.02; slow pathway, p less than 0.01), but did not alter the anterograde (n = 8) or retrograde (n = 9) refractory periods of accessory pathways. Flestolol prevented initiation of tachycardia by causing block in anterograde AV nodal conduction. It was more effective in patients with AV nodal tachycardia (5 of 6) than in those with AV reciprocating tachycardia (4 of 15, p less than 0.03). In patients in whom it was ineffective, the mean tachycardia cycle length increased by 54 ms because of an increase in AH interval (p less than 0.0001, n = 11). The cycle length of tachycardia induced 30 minutes after infusion was similar to the cycle length in the control state (354 vs 355 ms, n = 16). Flestolol's kinetics permitted clinically indicated electropharmacologic testing of a second antiarrhythmic drug in 8 patients and control of ventricular rate until arrhythmia surgery in 1 patient with incessant tachycardia. No hypotension or toxicity occurred. Our findings indicate that flestolol's principal antiarrhythmic effects are on the AV node, similar to the effects of other beta-blocking drugs. Its ultrashort duration of action is an advantage during electropharmacologic testing.

摘要

氟司洛尔是一种超短效β受体阻滞剂,半衰期为6.9分钟。对21例自发性和诱发性室上性心动过速患者(6例房室结性心动过速和15例房室折返性心动过速)研究了其抗心律失常疗效。它使所有房室结性心动过速患者的房室结有效不应期延长(快径路,p<0.02;慢径路,p<0.01),但未改变旁路的前向(n = 8)或逆向(n = 9)不应期。氟司洛尔通过阻滞房室结前向传导来预防心动过速的发作。它对房室结性心动过速患者(6例中的5例)比对房室折返性心动过速患者(15例中的4例,p<0.03)更有效。在无效的患者中,由于AH间期增加,平均心动过速周期长度增加了54毫秒(p<0.0001,n = 11)。输注后30分钟诱发的心动过速周期长度与对照状态下的周期长度相似(354对355毫秒,n = 16)。氟司洛尔的药代动力学特性允许对8例患者进行临床所需的第二种抗心律失常药物的电药理学测试,并对1例持续性心动过速患者在心律失常手术前控制心室率。未发生低血压或毒性反应。我们的研究结果表明,氟司洛尔的主要抗心律失常作用是作用于房室结,类似于其他β受体阻滞剂的作用。其超短的作用持续时间在电药理学测试中是一个优点。

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Electropharmacology of flestolol for supraventricular tachycardia without associated structural heart disease.氟司洛尔治疗无相关结构性心脏病的室上性心动过速的电药理学研究
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