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多非利特与美西律预防心房颤动的协同作用。

Synergistic Effect of Dofetilide and Mexiletine on Prevention of Atrial Fibrillation.

作者信息

Liu Guizhi, Xue Xiaolin, Gao Chuanyu, Huang Jiaqi, Qi Datun, Zhang Yanzhou, Dong Jian-Zeng, Ma Chang-Sheng, Yan Gan-Xin

机构信息

First Affiliated Hospital of Zhengzhou University, Zhengzhou, China.

Department of Cardiology, The First Affiliated Hospital, Xi'an Jiaotong University, Xi'an, China.

出版信息

J Am Heart Assoc. 2017 May 18;6(5):e005482. doi: 10.1161/JAHA.117.005482.

Abstract

BACKGROUND

Although atrial fibrillation (AF) is the most common abnormal heart rhythm and its prevalence continues to rise, there is a marked paucity of effective and safe antiarrhythmic drugs for AF. This study was done to test whether combined use of dofetilide and mexiletine exhibits not only a synergistic effect on AF suppression but also a safer profile in drug-induced ventricular proarrhythmias.

METHODS AND RESULTS

The effects of dofetilide plus mexiletine on atrial effective refractory period (ERP), AF inducibility, QT, and QT-related ventricular arrhythmias were studied using the isolated arterially perfused rabbit atrial and ventricular wedge preparations. Dofetilide or mexiletine alone mildly to moderately prolonged atrial ERP, but their combined use produced a markedly rate-dependent increase in atrial ERP. Dofetilide (3 nmol/L) plus mexiletine (10 μmol/L) increased the ERP by 28.2% from 72.2±5.7 to 92.8±5.9 ms (n=9, <0.01) at a pacing rate of 0.5 Hz and by 94.5% from 91.7±5.2 to 178.3±12.0 ms (n=9, <0.01) at 3.3 Hz. Dofetilide plus mexiletine strongly suppressed AF inducibility. On the other hand, dofetilide at 10 nmol/L produced marked QT and T prolongation, steeper QT-BCL and T-BCL slopes, and induced early afterdepolarizations and torsade de pointes in the ventricular wedges. Mexiletine at 10 μmol/L reduced dofetilide-induced QT and T prolongation, QT-BCL and T-BCL slopes, and abolished early afterdepolarizations and torsade de pointes.

CONCLUSIONS

In rabbits, combined use of dofetilide and mexiletine not only synergistically increases atrial ERP and effectively suppresses AF inducibility, but also markedly reduces QT liability and torsade de pointes risk posed by dofetilide alone.

摘要

背景

尽管心房颤动(AF)是最常见的心律失常,且其患病率持续上升,但用于治疗AF的有效且安全的抗心律失常药物却明显匮乏。本研究旨在测试多非利特与美西律联合使用是否不仅对AF抑制具有协同作用,而且在药物诱导的室性心律失常方面具有更安全的特征。

方法与结果

使用离体动脉灌注兔心房和心室楔形标本,研究了多非利特加美西律对心房有效不应期(ERP)、AF诱发率、QT以及QT相关室性心律失常的影响。单独使用多非利特或美西律可轻度至中度延长心房ERP,但它们联合使用可使心房ERP出现明显的频率依赖性增加。在起搏频率为0.5Hz时,多非利特(3nmol/L)加美西律(10μmol/L)使ERP从72.2±5.7ms增加到92.8±5.9ms,增幅为28.2%(n=9,P<0.01);在3.3Hz时,ERP从91.7±5.2ms增加到178.3±12.0ms,增幅为94.5%(n=9,P<0.01)。多非利特加美西律强烈抑制AF诱发率。另一方面,10nmol/L的多非利特可使心室楔形标本出现明显的QT和T波延长、更陡峭的QT-心动周期长度(BCL)和T-BCL斜率,并诱发早期后除极和尖端扭转型室性心动过速。10μmol/L的美西律可减少多非利特诱导的QT和T波延长、QT-BCL和T-BCL斜率,并消除早期后除极和尖端扭转型室性心动过速。

结论

在兔体内,多非利特与美西律联合使用不仅可协同增加心房ERP并有效抑制AF诱发率,而且可显著降低多非利特单独使用时的QT相关风险和尖端扭转型室性心动过速风险。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26c3/5524094/bad42e5d46a9/JAH3-6-e005482-g001.jpg

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