基因消融TASK-1(弱内向整流K+通道相关酸敏感K+通道-1中P结构域串联)(K2P3.1) K+通道抑制心房颤动并防止电重构

Circulation: Arrhythmia and Electrophysiology Pub Date : 2019-09-01 DOI:10.1161/CIRCEP.119.007465

C. Schmidt, F. Wiedmann, C. Beyersdorf, Zhihan Zhao, I. El-Battrawy, H. Lan, G. Szabó, Xin Li, S. Lang, S. Korkmaz‐Icöz, K. Rapti, A. Jungmann, Antonius Ratte, O. Müller, M. Karck, G. Seemann, I. Akin, M. Borggrefe, Xiaobo Zhou, H. Katus, Dierk Thomas

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引用次数: 25

摘要

背景:尽管对房颤(AF)病理生理的了解越来越多，但缺乏转化为基于机制的治疗选择。在慢性房颤患者心房心肌细胞中，弱内向整流TASK-1 (K+通道相关的酸敏感K+通道-1)(K2P3.1)心房特异性2孔结构域钾通道中P结构域串联表达和功能增强，导致动作电位持续时间缩短。TASK-1通道抑制阻止动作电位持续时间缩短以维持在窦性心律受试者中观察到的值。本临床前研究采用猪房颤模型来评估腺相关病毒抗TASK-1 sirna(小干扰RNA)基因转移抑制TASK-1的抗心律失常效果。方法采用植入心脏起搏器的心房爆裂刺激法诱导家猪心房颤动。将携带抗TASK-1 sirna的腺相关病毒载体注射到双心房以抑制TASK-1通道的表达。随访14 d后，分别从猪左右心房分离心肌细胞，进行电生理和分子表征。结果:与窦性心律对照相比，saf与增加的TASK-1转录物、蛋白和离子电流水平相关，导致心房心肌细胞动作电位持续时间缩短，与先前在人类中的发现相似。与未经治疗的AF猪相比，抗task -1腺相关病毒的应用显著降低了AF猪的负担。抗TASK-1- sirna的抗心律失常作用与减少TASK-1电流和延长心房心肌细胞的动作电位持续时间至窦性心律值有关。结论基于腺相关病毒的抗TASK-1基因治疗在猪房颤模型中抑制房颤并纠正细胞电生理重构。通过选择性减少TASK-1电流抑制房颤是抗心律失常治疗的新选择。

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Genetic Ablation of TASK-1 (Tandem of P Domains in a Weak Inward Rectifying K+ Channel-Related Acid-Sensitive K+ Channel-1) (K2P3.1) K+ Channels Suppresses Atrial Fibrillation and Prevents Electrical Remodeling.

BACKGROUND Despite an increasing understanding of atrial fibrillation (AF) pathophysiology, translation into mechanism-based treatment options is lacking. In atrial cardiomyocytes of patients with chronic AF, expression, and function of tandem of P domains in a weak inward rectifying TASK-1 (K+ channel-related acid-sensitive K+ channel-1) (K2P3.1) atrial-specific 2-pore domain potassium channels is enhanced, resulting in action potential duration shortening. TASK-1 channel inhibition prevents action potential duration shortening to maintain values observed among sinus rhythm subjects. The present preclinical study used a porcine AF model to evaluate the antiarrhythmic efficacy of TASK-1 inhibition by adeno-associated viral anti-TASK-1-siRNA (small interfering RNA) gene transfer. METHODS AF was induced in domestic pigs by atrial burst stimulation via implanted pacemakers. Adeno-associated viral vectors carrying anti-TASK-1-siRNA were injected into both atria to suppress TASK-1 channel expression. After the 14-day follow-up period, porcine cardiomyocytes were isolated from right and left atrium, followed by electrophysiological and molecular characterization. RESULTS AF was associated with increased TASK-1 transcript, protein and ion current levels leading to shortened action potential duration in atrial cardiomyocytes compared to sinus rhythm controls, similar to previous findings in humans. Anti-TASK-1 adeno-associated viral application significantly reduced AF burden in comparison to untreated AF pigs. Antiarrhythmic effects of anti-TASK-1-siRNA were associated with reduction of TASK-1 currents and prolongation of action potential durations in atrial cardiomyocytes to sinus rhythm values. Conclusions Adeno-associated viral-based anti-TASK-1 gene therapy suppressed AF and corrected cellular electrophysiological remodeling in a porcine model of AF. Suppression of AF through selective reduction of TASK-1 currents represents a new option for antiarrhythmic therapy.

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Circulation: Arrhythmia and Electrophysiology

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