Etheridge Susan P, Compton Steven J, Tristani-Firouzi Martin, Mason Jay W
Primary Children's Medical Center and the Division of Pediatric Cardiology, University of Utah School of Medicine, Salt Lake City, Utah 84113, USA.
J Am Coll Cardiol. 2003 Nov 19;42(10):1777-82. doi: 10.1016/j.jacc.2003.07.006.
We sought to determine whether oral potassium supplementation safely increases serum K(+) and results in sustained improvement of repolarization parameters in long QT syndrome type 2 (LQT2) subjects.
Mutations in HERG (LQT2), the gene encoding the rapid delayed rectifier K(+) current I(Kr), account for a significant proportion of congenital long QT syndrome (LQTS). The magnitude of I(Kr) is paradoxically increased by an increase in extracellular K(+). We tested the hypothesis that long-term oral potassium supplementation results in a mild, sustainable increase in serum K(+) that improves repolarization abnormalities in subjects with LQT2.
After an initial evaluation consisting of electrocardiography, electrolytes, blood urea nitrogen, and creatinine, escalating doses of potassium chloride (KCl) and spironolactone were administered to eight subjects with six distinct HERG mutations. Medications were continued for four weeks, at which time, the final evaluation was undertaken. Beta-adrenergic blocking therapy was maintained.
The subjects ranged in age from 11 to 52 years. The average daily KCl and spironolactone dose was 3.3 +/- 1.5 mEq/kg and 3.5 +/- 1.2 mg/kg, respectively, and this regimen resulted in an increase in serum K(+) from 4.0 +/- 0.3 to 5.2 +/- 0.3 mEq/l. There were no serious complications associated with therapy. The increase in serum K(+) resulted in a decrease in the corrected QT interval from 526 +/- 94 to 423 +/- 36 ms (mean +/- SD; lead V(2)). Both QT dispersion and T-wave morphology improved in most subjects.
Long-term oral potassium administration increases serum K(+) in patients with LQT2. This can be achieved safely and results in improvement in repolarization. Further studies are warranted to determine whether this will reduce the incidence of life-threatening events in LQTS patients.
我们试图确定口服补钾是否能安全地提高血清钾水平,并使2型长QT综合征(LQT2)患者的复极参数得到持续改善。
编码快速延迟整流钾电流I(Kr)的HERG基因(LQT2)突变在先天性长QT综合征(LQTS)中占很大比例。细胞外钾离子浓度升高时,I(Kr)的幅度反而会增加。我们检验了这样一个假设,即长期口服补钾会使血清钾水平出现轻度、持续的升高,从而改善LQT2患者的复极异常。
在进行包括心电图、电解质、血尿素氮和肌酐在内的初始评估后,对8名携带6种不同HERG突变的患者给予递增剂量的氯化钾(KCl)和螺内酯。药物持续服用4周,届时进行最终评估。β肾上腺素能阻滞剂治疗持续进行。
患者年龄在11至52岁之间。氯化钾和螺内酯的平均每日剂量分别为3.3±1.5 mEq/kg和3.5±1.2 mg/kg,该方案使血清钾从4.0±0.3 mEq/l升高至5.2±0.3 mEq/l。治疗未出现严重并发症。血清钾升高导致校正QT间期从526±94毫秒降至423±36毫秒(平均值±标准差;V(2)导联)。大多数患者的QT离散度和T波形态均有所改善。
长期口服补钾可使LQT2患者的血清钾升高。这一过程可安全实现,并能改善复极情况。有必要进一步研究以确定这是否会降低LQTS患者危及生命事件的发生率。
