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氟卡尼对携带新SCN5A突变患者的影响:长QT综合征的突变特异性治疗?

Effects of flecainide in patients with new SCN5A mutation: mutation-specific therapy for long-QT syndrome?

作者信息

Benhorin J, Taub R, Goldmit M, Kerem B, Kass R S, Windman I, Medina A

机构信息

Department of Cardiology, Bikur Cholim Hospital, Jerusalem, Israel.

出版信息

Circulation. 2000 Apr 11;101(14):1698-706. doi: 10.1161/01.cir.101.14.1698.

DOI:10.1161/01.cir.101.14.1698
PMID:10758053
Abstract

BACKGROUND

Mutations in the cardiac sodium channel gene (SCN5A) can cause one variant of the congenital long-QT syndrome. The effects of some of these mutations on the alpha-subunit channel properties can be blocked by type Ib antiarrhythmic drugs. Recently, we have described a new SCN5A mutation (D1790G) that affects the channel properties in a manner suggesting that sodium blockers of the Ib type will be ineffective in carriers of this mutation. Hence, the ECG effects of flecainide-acetate, a type Ic sodium blocker, were evaluated in carriers of this mutation.

METHODS AND RESULTS

Eight asymptomatic mutation carriers and 5 control subjects were studied. Intravenous lidocaine was tested first in only 2 mutation carriers and had no significant effect on any ECG parameter. Flecainide significantly shortened all heart rate-corrected repolarization duration parameters only in carriers and not in control subjects: QT(c) shortened by 9.5% (from 517+/-45 to 468+/-36 ms, P=0.011), and the S-offset to T-onset interval shortened by 64.7% (from 187+/-88 to 66+/-50 ms, P=0.0092). Flecainide also normalized the marked baseline repolarization dispersion in most mutation carriers. These effects among carriers were maintained during long-term (9 to 17 months) outpatient flecainide therapy with no adverse effects.

CONCLUSIONS

This report is the first to describe SCN5A mutation carriers who significantly responded to flecainide therapy yet did not respond to lidocaine. These results have important implications for long-QT allele-specific therapeutic strategies.

摘要

背景

心脏钠通道基因(SCN5A)突变可导致先天性长QT综合征的一种变异型。Ib类抗心律失常药物可阻断其中一些突变对α亚基通道特性的影响。最近,我们描述了一种新的SCN5A突变(D1790G),其对通道特性的影响表明Ib型钠通道阻滞剂对该突变携带者无效。因此,我们评估了Ic类钠通道阻滞剂醋酸氟卡尼对该突变携带者的心电图影响。

方法与结果

研究了8名无症状突变携带者和5名对照者。仅对2名突变携带者首先进行了静脉注射利多卡因试验,对任何心电图参数均无显著影响。醋酸氟卡尼仅使携带者的所有心率校正复极持续时间参数显著缩短,而对照者则无此现象:QTc缩短了9.5%(从517±45毫秒缩短至468±36毫秒,P = 0.011),S波起点至T波起点间期缩短了64.7%(从187±88毫秒缩短至66±50毫秒,P = 小括号0.0092)。醋酸氟卡尼还使大多数突变携带者明显的基线复极离散度恢复正常。在长期(9至17个月)门诊醋酸氟卡尼治疗期间,携带者中的这些效应得以维持,且无不良反应。

结论

本报告首次描述了对醋酸氟卡尼治疗有显著反应但对利多卡因无反应的SCN5A突变携带者。这些结果对长QT等位基因特异性治疗策略具有重要意义。

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