独特的心脏浦肯野纤维瞬间外向电流β亚基组成:特发性心室颤动的潜在分子联系。
Unique cardiac Purkinje fiber transient outward current β-subunit composition: a potential molecular link to idiopathic ventricular fibrillation.
机构信息
Department of Medicine, Montreal Heart Institute and Université de Montréal, Montreal, QC, Canada.
出版信息
Circ Res. 2013 May 10;112(10):1310-22. doi: 10.1161/CIRCRESAHA.112.300227. Epub 2013 Mar 26.
RATIONALE
A chromosomal haplotype producing cardiac overexpression of dipeptidyl peptidase-like protein-6 (DPP6) causes familial idiopathic ventricular fibrillation. The molecular basis of transient outward current (I(to)) in Purkinje fibers (PFs) is poorly understood. We hypothesized that DPP6 contributes to PF I(to) and that its overexpression might specifically alter PF I(to) properties and repolarization.
OBJECTIVE
To assess the potential role of DPP6 in PF I(to).
METHODS AND RESULTS
Clinical data in 5 idiopathic ventricular fibrillation patients suggested arrhythmia origin in the PF-conducting system. PF and ventricular muscle I(to) had similar density, but PF I(to) differed from ventricular muscle in having tetraethylammonium sensitivity and slower recovery. DPP6 overexpression significantly increased, whereas DPP6 knockdown reduced, I(to) density and tetraethylammonium sensitivity in canine PF but not in ventricular muscle cells. The K(+)-channel interacting β-subunit K(+)-channel interacting protein type-2, essential for normal expression of I(to) in ventricular muscle, was weakly expressed in human PFs, whereas DPP6 and frequenin (neuronal calcium sensor-1) were enriched. Heterologous expression of Kv4.3 in Chinese hamster ovary cells produced small I(to); I(to) amplitude was greatly enhanced by coexpression with K(+)-channel interacting protein type-2 or DPP6. Coexpression of DPP6 with Kv4.3 and K(+)-channel interacting protein type-2 failed to alter I(to) compared with Kv4.3/K(+)-channel interacting protein type-2 alone, but DPP6 expression with Kv4.3 and neuronal calcium sensor-1 (to mimic PF I(to) composition) greatly enhanced I(to) compared with Kv4.3/neuronal calcium sensor-1 and recapitulated characteristic PF kinetic/pharmacological properties. A mathematical model of cardiac PF action potentials showed that I(to) enhancement can greatly accelerate PF repolarization.
CONCLUSIONS
These results point to a previously unknown central role of DPP6 in PF I(to), with DPP6 gain of function selectively enhancing PF current, and suggest that a DPP6-mediated PF early-repolarization syndrome might be a novel molecular paradigm for some forms of idiopathic ventricular fibrillation.
背景
一种导致家族性特发性心室颤动的二肽基肽酶样蛋白-6(DPP6)的染色体单倍型可导致心脏过表达。浦肯野纤维(PF)中的瞬时外向电流(I(to))的分子基础尚未完全清楚。我们假设 DPP6 有助于 PF I(to),并且其过表达可能会特异性改变 PF I(to)的特性和复极化。
目的
评估 DPP6 在 PF I(to)中的潜在作用。
方法和结果
5 名特发性心室颤动患者的临床数据表明,心律失常起源于 PF 传导系统。PF 和心室肌 I(to)的密度相似,但 PF I(to)与心室肌不同,具有四乙基铵敏感性和较慢的恢复。DPP6 过表达显著增加,而 DPP6 敲低则降低了犬 PF 中的 I(to)密度和四乙基铵敏感性,但不降低心室肌细胞中的 I(to)密度和四乙基铵敏感性。对于心室肌中正常表达 I(to)至关重要的 K+通道相互作用β亚基 K+通道相互作用蛋白 2 在人 PF 中表达较弱,而 DPP6 和 frequenin(神经元钙传感器-1)丰富。在中国仓鼠卵巢细胞中异源表达 Kv4.3 产生的 I(to)较小;当与 K+通道相互作用蛋白 2 或 DPP6 共表达时,I(to)幅度大大增强。与 Kv4.3/K+通道相互作用蛋白 2 单独共表达 DPP6 对 I(to)没有改变,但 Kv4.3 与神经元钙传感器-1(模拟 PF I(to)组成)共表达大大增强了 I(to),与 Kv4.3/神经元钙传感器-1 相比,大大增强了 I(to),并再现了特征性的 PF 动力学/药理学特性。心脏 PF 动作电位的数学模型表明,I(to)增强可以大大加速 PF 复极。
结论
这些结果表明 DPP6 在 PF I(to)中具有以前未知的核心作用,DPP6 功能获得选择性增强 PF 电流,并表明 DPP6 介导的 PF 早期复极化综合征可能是某些形式的特发性心室颤动的一种新的分子范例。
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