Akar Fadi G, Yan Gan-Xin, Antzelevitch Charles, Rosenbaum David S
Heart and Vascular Research Center and Departments of Medicine and Biomedical Engineering, Case Western Reserve University, Cleveland, Ohio 44109-1998, USA.
Circulation. 2002 Mar 12;105(10):1247-53. doi: 10.1161/hc1002.105231.
Specific ion channel mutations underlie the congenital long-QT syndrome (LQTS). However, the mechanisms by which dysfunction at the molecular level translates into functional electrical instability leading to torsade de pointes (TdP) in LQTS are poorly understood.
The cellular basis of TdP was investigated using a novel approach of transmural optical imaging in the canine wedge preparation (n=14). The spatial organization of repolarization and arrhythmogenesis were determined in a surrogate model of LQT2. Action potentials were recorded simultaneously from 128 sites spanning the transmural wall of the left ventricle. In LQT2, QT interval prolongation was paralleled by an abrupt rise in transmural dispersion of repolarization (DOR) from 2.7 plus/minus 0.9 ms/mm (controls) to 12.2 plus/minus 2.1 ms/mm (LQT2). Islands of midmyocardial (M) cells formed zones of increased refractoriness in LQT2, producing steep spatial gradients of repolarization that were directly responsible for conduction block and self-sustained intramural reentrant circuits underlying TdP.
These data provide direct evidence supporting the functional expression of M cells in intact myocardium and a central role for M cells in the development of reentrant TdP arrhythmias in LQTS.
特定离子通道突变是先天性长QT综合征(LQTS)的基础。然而,分子水平的功能障碍如何转化为导致LQTS中尖端扭转型室速(TdP)的功能性电不稳定的机制尚不清楚。
采用一种新的犬楔形标本透壁光学成像方法(n = 14)研究TdP的细胞基础。在LQT2替代模型中确定复极化的空间组织和心律失常的发生机制。从跨越左心室透壁壁的128个部位同时记录动作电位。在LQT2中,QT间期延长的同时,复极化跨壁离散度(DOR)从2.7±0.9毫秒/毫米(对照组)突然增加到12.2±2.1毫秒/毫米(LQT2)。中层心肌(M)细胞岛在LQT2中形成了不应期增加的区域,产生了陡峭的复极化空间梯度,这直接导致了传导阻滞和TdP潜在的自维持壁内折返环。
这些数据提供了直接证据,支持M细胞在完整心肌中的功能表达以及M细胞在LQTS折返性TdP心律失常发生中的核心作用。
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