Regulation of cardiac repolarization by adenoviral gene transfer rationalized by computational modeling

R. Mazhari, E. Marbán, R. Winslow
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引用次数: 0

Abstract

Regulatory subunit KCNE3 (E3) interacts with KCNQ1 (Q1) in epithelia, regulating its activation kinetics and augmenting current density. Since E3 is expressed weakly in the heart, we hypothesized that ectopic expression of E3 in cardiac myocytes might abbreviate action potential duration by interacting with Q1 and augmenting the delayed rectifier current (I/sub K/). We constructed an adenoviral vector co-expressing GFP and E3, and injected it Into the left ventricular cavity of guinea pigs. After 72 hrs, the electrocardiographic QT interval was reduced by /spl sim/10% compared to baseline. E3-transduced cells had an APD/sub 90/ of 87 /spl plusmn/ 8 vs. 298 /spl plusmn/ 19 ms in control cells, while E-4031-insensitive I/sub K/ and activation kinetics were significantly augmented. Quantitative modeling of a transmural cardiac segment rationalized the degree of QT-interval abbreviation as a consequence of electrotonic interactions in the face of limited transduction efficiency and showed that heterogeneous transduction of E3 may actually potentiate arrhythmias. The results provide proof of the principle that ectopic expression of regulatory subunits can be exploited to enhance repolarization, a principle that may be useful in treating long QT syndrome (but only if fairly homogeneous ventricular expression can be achieved).
计算模型证明了腺病毒基因转移对心脏复极化的调节作用
调控亚基KCNE3 (E3)与上皮细胞中的KCNQ1 (Q1)相互作用,调节其激活动力学并增加电流密度。由于E3在心脏中的表达较弱,我们假设E3在心肌细胞中的异位表达可能通过与Q1相互作用并增加延迟整流电流(I/sub K/)而缩短动作电位持续时间。构建了GFP与E3共表达的腺病毒载体,并将其注入豚鼠左心室。72小时后,心电图QT间期与基线相比减少了10%。e3转导细胞的APD/sub 90/为87 /spl plusmn/ 8,而对照组细胞的APD/sub 90/为298 /spl plusmn/ 19 ms,而e -4031不敏感细胞的I/sub K/和活化动力学显著增强。跨壁心脏段的定量建模合理化了面对有限转导效率的电紧张相互作用导致的qt间期缩短的程度,并表明E3的异质性转导实际上可能加剧心律失常。结果证明了调控亚基的异位表达可以增强复极,这一原理可能对治疗长QT综合征有用(但前提是能够实现相当均匀的心室表达)。
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