美西律缩短钾通道介导的 2 型长 QT 综合征患者的 QT 间期。
Mexiletine Shortens the QT Interval in Patients With Potassium Channel-Mediated Type 2 Long QT Syndrome.
机构信息
Division of Pediatric Cardiology, Department of Pediatric and Adolescent Medicine (J.M.B., R.K.R., M.J.A.), Mayo Clinic, Rochester, MN.
Department of Molecular Pharmacology and Experimental Therapeutics (Windland Smith Rice Sudden Death Genomics Laboratory) (J.M.B., M.J.A.), Mayo Clinic, Rochester, MN.
出版信息
Circ Arrhythm Electrophysiol. 2019 May;12(5):e007280. doi: 10.1161/CIRCEP.118.007280.
BACKGROUND
Long QT syndrome is a potentially lethal yet highly treatable cardiac channelopathy. Although β-blocker therapy is standard for most patients, concomitant therapy with sodium channel blockers, like mexiletine, is often utilized for patients with sodium channel-mediated type 3 long QT syndrome (LQT3). The potential role of sodium channel blockers in patients with potassium channel-mediated long QT syndrome (ie, LQT1 and LQT2) has not been investigated in detail.
METHODS
We performed a retrospective chart review on 12 patients (5 females; median age at diagnosis 14.1 years (interquartile range [IQR], 7.7-23; range, 0-59, median heart rate-corrected QT interval [QTc] at diagnosis 557 ms (IQR, 529-605) with genetically established LQT2 (10) or a combination of LQT1/LQT2 (1) or LQT2/LQT3 (1), who received mexiletine. Data were collected on symptomatic status, treatments, and breakthrough cardiac events after diagnosis and initiation of treatment. Additionally, 12-lead ECGs were collected at diagnosis, before initiation of mexiletine and following mexiletine to evaluate the drug's effect on QTc.
RESULTS
Before diagnosis, 6 patients were symptomatic and, before initiation of mexiletine, 4 patients experienced ≥1 breakthrough cardiac event on β-blocker. Median age at first mexiletine dose was 24.3 years (IQR, 14-32.4). After mexiletine, the median QTc decreased by 65±45 ms from 547 ms (IQR, 488-558) premexiletine to 470 ms (IQR, 409-529) postmexiletine ( P=0.0005) for all patients. In 8 patients (67%), the QTc decreased by ≥ 40 ms with a mean decrease in QTc of 91 ms ( P < 0.008). For the 11 patients maintained on mexiletine therapy, there have been no breakthrough cardiac events during follow-up.
CONCLUSIONS
Although commonly prescribed in patients with LQT3, mexiletine also shortens the QTc significantly in two-thirds of a small subset of patients with potassium channel-mediated LQT2. In patients with LQT2, pharmacological targeting of the physiological late sodium current may provide added therapeutic efficacy to β-blocker therapy.
背景
长 QT 综合征是一种潜在致命但高度可治疗的心脏通道病。尽管β受体阻滞剂治疗是大多数患者的标准治疗方法,但对于钠离子通道介导的 3 型长 QT 综合征(LQT3)患者,常同时使用钠离子通道阻滞剂,如美西律。钠离子通道阻滞剂在钾离子通道介导的长 QT 综合征(即 LQT1 和 LQT2)患者中的潜在作用尚未详细研究。
方法
我们对 12 名患者(5 名女性;中位诊断年龄为 14.1 岁(四分位间距[IQR],7.7-23;范围,0-59),中位诊断时校正后的 QT 间期[QTc]为 557 ms(IQR,529-605),具有遗传确立的 LQT2(10 例)或 LQT1/LQT2 联合(1 例)或 LQT2/LQT3(1 例),接受美西律治疗。收集诊断后和治疗开始后症状状态、治疗和突破性心脏事件的数据。此外,在诊断时、开始使用美西律之前和使用美西律后收集 12 导联心电图,以评估药物对 QTc 的影响。
结果
在诊断之前,有 6 名患者有症状,在开始使用美西律之前,有 4 名患者在使用β受体阻滞剂时发生了≥1 次突破性心脏事件。首次美西律剂量的中位年龄为 24.3 岁(IQR,14-32.4)。使用美西律后,所有患者的 QTc 从美西律前的 547 ms(IQR,488-558)降至 470 ms(IQR,409-529)(P=0.0005),中位数降低 65±45 ms。在 8 名(67%)患者中,QTc 降低≥40 ms,平均降低 91 ms(P<0.008)。在 11 名继续接受美西律治疗的患者中,在随访期间没有发生突破性心脏事件。
结论
尽管在 LQT3 患者中通常使用美西律,但它还可使钾离子通道介导的 LQT2 患者中的小部分患者的 QTc 显著缩短。在 LQT2 患者中,针对生理晚期钠电流的药理学靶向治疗可能为β受体阻滞剂治疗提供额外的治疗效果。
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