首页> 外文期刊>British Journal of Clinical Pharmacology >Intravenous antazoline, a first-generation antihistaminic drug with antiarrhythmic properties, is a suitable agent for pharmacological cardioversion of atrial fibrillation induced during pulmonary vein isolation due to the lack of influence on atrio-venous conduction and high clinical effectiveness (AntaEP Study)
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Intravenous antazoline, a first-generation antihistaminic drug with antiarrhythmic properties, is a suitable agent for pharmacological cardioversion of atrial fibrillation induced during pulmonary vein isolation due to the lack of influence on atrio-venous conduction and high clinical effectiveness (AntaEP Study)

机译:静脉内抗唑啉,一种具有抗心律失常性的第一代抗氨胺类药物,是在肺静脉隔离期间诱导的心房颤动的药理心脏药物心脏病药物的合适试剂由于缺乏对大静脉传导和高临床效果(ANSEP研究)的影响而造成的肺静脉分离

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Aims Antazoline is a first-generation antihistaminic drug used primarily in eye drop formulations. When administered intravenously, antazoline displays antiarrhythmic properties resulting in a rapid conversion of recent-onset atrial fibrillation (AF) to sinus rhythm (SR). The aim of the study was to assess the influence of antazoline on atrio-venous conduction and other electrophysiological parameters in patients undergoing AF ablation. Methods An experimental prospective study. Patients scheduled for the first-time AF ablation, in SR and not on amiodarone were enrolled. Atrio-venous conduction assessment and invasive electrophysiological study (EPS) were performed before and after intravenous administration of 250 mg of antazoline. In case of AF induction during EPS, antazoline was administered until conversion to SR or a cumulative dose of 300 mg. Results We enrolled 14 patients: 13 (93%) men, mean age 63.4 (59.9-66.8) years, mean CHA(2)DS(2)-VASc score 1.6 (1.0-2.2). Antazoline was administered in a mean dose 257.1 (246.7-267.6) mg. Pulmonary vein potentials and atrial capture during pulmonary vein stimulation were present before and after the administration of antazoline. Wenckebach point and atrial conduction times did not change significantly, but atrio-ventricular node effective refractory period improved-324.7 (275.9-373.5) ms vs 284.3 (256.2-312.4) ms, P = 0.02. Antazoline was effective in all 5 (100%) cases of AF induction during EPS. There were no serious adverse events. Conclusion Due to the lack of influence on atrio-venous conduction and high clinical effectiveness, antazoline may be suitable for pharmacological cardioversion of AF occurring during AF ablation.
机译:AIMS抗唑啉是一种主要用于眼药滴制剂的第一代抗组胺药药物。当静脉内施用时,抗唑啉显示抗心律失常的性质,导致急剧转化的近期出现的心房颤动(AF)至窦性心律(SR)。该研究的目的是评估抗唑啉对AF消融患者患者的大静脉传导和其他电生理学参数的影响。方法实验前瞻性研究。患者安排为第一次AF消融,在SR中纳入胺碘酮。在静脉内施用250mg抗唑啉之前和之后进行大静脉传导评估和侵入式电生理学研究(EPS)。在EPS期间的AF诱导的情况下,施用抗唑啉直至转化为SR或300mg的累积剂量。结果我们注册了14名患者:13例(93%)男性,平均63.4岁(59.9-66.8)年,平均CHA(2)DS(2)-VASC得分1.6(1.0-2.2)。抗唑啉以平均剂量257.1(246.7-267.6)Mg施用。肺静脉刺激期间的肺静脉电位和心房捕获存在于抗唑啉施用之前和之后。 WENCKEBACH点和心房传导时间没有显着变化,但Atrio-心室节点有效的耐火剂改善-324.7(275.9-373.5)MS VS 284.3(256.2-312.4)MS,P = 0.02。抗唑啉在EPS期间的所有5(100%)AF诱导的情况下都是有效的。没有严重的不良事件。结论由于对大静脉传导的影响缺乏影响和高临床效果,抗唑啉适用于AF消融期间发生的AF的药理心脏病。

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