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房室结内 I(f)电流抑制是决奈达隆降低心房颤动心室率的机制。

Inhibition of I(f) in the atrioventricular node as a mechanism for dronedarone's reduction in ventricular rate during atrial fibrillation.

机构信息

Beth Israel Deaconess Medical Center and; Harvard Medical School, Boston, Massachusetts.

出版信息

Heart Rhythm. 2013 Nov;10(11):1692-7. doi: 10.1016/j.hrthm.2013.08.007. Epub 2013 Aug 9.

Abstract

BACKGROUND

In clinical trials, dronedarone lowers ventricular rate during atrial fibrillation (AF). This agent was recently demonstrated to inhibit If in the sinoatrial node.

OBJECTIVE

The purpose of this study was to examine whether dronedarone inhibits If at the atrioventricular (AV) node to reduce ventricular rate during AF by slowing conduction at the AV node.

METHODS

We studied the effects of dronedarone (1.0 mg/kg IV bolus) before and after administration of the If inhibitor ivabradine (0.5 mg/kg IV). Ventricular rate, mean arterial pressure, dominant frequency of AF, PR and QT intervals, and atrial (AERP) and ventricular effective refractory periods (VERP) were measured during atrial pacing at 150 bpm in an anesthetized pig model of AF induced by intrapericardial acetylcholine and burst pacing.

RESULTS

Dronedarone reduced ventricular rate during AF by 22.1% (from 213 ± 11.1 bpm to 166 ± 8.3 bpm, P = .01) and increased PR interval by 8.7% (from 173 ± 5.6 ms to 188 ± 5.2 ms, P = .001), QT interval by 3.3% (from 272 ± 6.2 ms to 281 ± 4.9 ms, P = .05), and AERP and VERP by 6.2% and 11.7%, respectively. All other parameters remained unchanged. Dronedarone plasma levels were low (29 ± 4 nM), and concentration in tissue was 15- to 21-fold higher than in plasma. Ivabradine reduced ventricular rate during AF by 39.5% (from 200 ± 14.6 bpm to 121 ± 20.1 bpm, P = .005) and increased PR interval by 20.4% (from 157 ± 9.5 ms to 189 ± 7.4 ms, P <.05). Administration of dronedarone after ivabradine did not further alter these endpoints.

CONCLUSION

Dronedarone, which is concentrated in myocardial tissue, reduces ventricular rate during AF by slowing AV conduction. Absence of this effect after ivabradine administration implicates If inhibition as a mechanism.

摘要

背景

在临床试验中,决奈达隆可降低心房颤动(AF)时的心室率。该药物最近被证明可抑制窦房结中的 If。

目的

本研究的目的是研究决奈达隆是否通过减慢房室(AV)结传导来抑制 AV 结的 If,从而降低 AF 时的心室率。

方法

我们在经心包内乙酰胆碱和burst 起搏诱导的 AF 猪模型中,在 150 bpm 的心房起搏下,研究了决奈达隆(1.0 mg/kg 静脉推注)给药前后 If 抑制剂伊伐布雷定(0.5 mg/kg 静脉推注)的作用。在麻醉猪模型中,在 150 bpm 的心房起搏下,测量心室率、平均动脉压、AF 的优势频率、PR 间期和 QT 间期以及心房(AERP)和心室有效不应期(VERP)。

结果

决奈达隆使 AF 时的心室率降低了 22.1%(从 213±11.1 bpm 降至 166±8.3 bpm,P=0.01),并使 PR 间期延长 8.7%(从 173±5.6 ms 增至 188±5.2 ms,P=0.001),QT 间期延长 3.3%(从 272±6.2 ms 增至 281±4.9 ms,P=0.05),AERP 和 VERP 分别延长 6.2%和 11.7%。其他所有参数均无变化。决奈达隆的血药浓度较低(29±4 nM),而组织浓度是血浆浓度的 15-21 倍。伊伐布雷定使 AF 时的心室率降低了 39.5%(从 200±14.6 bpm 降至 121±20.1 bpm,P=0.005),并使 PR 间期延长 20.4%(从 157±9.5 ms 增至 189±7.4 ms,P<.05)。伊伐布雷定给药后给予决奈达隆并未进一步改变这些终点。

结论

决奈达隆在心肌组织中浓集,通过减慢 AV 传导来降低 AF 时的心室率。伊伐布雷定给药后无此作用提示 If 抑制是一种机制。

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