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安他唑啉用于在旁路消融术中快速终止房颤。

Antazoline for rapid termination of atrial fibrillation during ablation of accessory pathways.

作者信息

Piotrowski Roman, Kryński Tomasz, Baran Jakub, Futyma Piotr, Stec Sebastian, Kułakowski Piotr

机构信息

Department of Cardiology, Grochowski Hospital, Postgraduate Medical School, Warsaw, Poland.

出版信息

Cardiol J. 2014;21(3):299-303. doi: 10.5603/CJ.a2013.0121. Epub 2013 Aug 30.

Abstract

BACKGROUND AND AIM

To assess safety and efficacy of antazoline for termination of atrial fibrillation (AF) occurring during ablation of accessory pathways (AP).

METHODS

We analyzed electrophysiological mechanism of antazoline (changes in A-A interval) and the percentage of pre-excited QRS complexes before and after antazoline administration. The total dose administered and the time from the start of injection to sinus rhythm restoration were also measured.

RESULTS

Out of consecutive 290 patients with Wolff-Parkinson-White syndrome undergoing radiofrequency (RF) ablation, 12 (4.1%) (4 females, mean age 36 ± 20 years) developed sustained AF which did not stop spontaneously within 10 min, and antazoline in 100 mg repeated boluses was administered. In all 12 patients the drug restored sinus rhythm after a mean of 425 ± 365 s (range 43-1245 s) using a mean cumulative dose of 176 ± 114 mg (range 25-400 mg). The drug slightly prolonged R-R intervals during AF (from 383 ± 106 to 410 ± 70 ms) and reduced the percentage of fully pre-excited QRS complexes (from 35% to 26%). Intracardiac recordings showed gradual increase in A-A intervals, as well as regularization and decreasing fractionation of atrial activity following drug injection (mean A-A interval of 162 ± 30 ms at baseline vs. 226 ± 26 ms shortly before sinus rhythm restoration, p < 0.001). AP was not completely blocked in any patient which enabled continuation of ablation.

CONCLUSIONS

Antazoline safely and rapidly converts AF into sinus rhythm during ablation of AP. The drug does not block AP completely, enabling continuation of ablation. The drug converting AF into more organized atrial activity (atrial flutter/tachycardia) before sinus rhythm resumption.

摘要

背景与目的

评估安他唑啉用于终止房室旁道(AP)消融过程中发生的房颤(AF)的安全性和有效性。

方法

我们分析了安他唑啉的电生理机制(A-A间期变化)以及给药前后预激QRS波群的百分比。还测量了给药总量以及从开始注射到恢复窦性心律的时间。

结果

在连续290例接受射频(RF)消融的 Wolff-Parkinson-White综合征患者中,12例(4.1%)(4例女性,平均年龄36±20岁)发生了持续性房颤,且在10分钟内未自行终止,给予100mg重复推注的安他唑啉。在所有12例患者中,该药物平均在425±365秒(范围43 - 1245秒)后恢复窦性心律,平均累积剂量为176±114mg(范围25 - 400mg)。该药物在房颤期间略微延长了R-R间期(从383±106毫秒延长至410±70毫秒),并降低了完全预激QRS波群的百分比(从35%降至26%)。心内记录显示,注射药物后A-A间期逐渐增加,心房活动逐渐规则化且碎裂程度降低(窦性心律恢复前不久平均A-A间期为226±26毫秒,而基线时为162±30毫秒,p < 0.001)。在任何患者中AP均未被完全阻断,从而能够继续进行消融。

结论

在AP消融过程中,安他唑啉能安全、迅速地将房颤转为窦性心律。该药物不会完全阻断AP,从而能够继续进行消融。该药物在窦性心律恢复前将房颤转为更规整的心房活动(心房扑动/心动过速)。

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