L型钙通道拮抗作用对携带模拟人类长QT综合征3型Scn5a基因突变的小鼠心脏室性心律失常发生的影响。
Effects of L-type Ca2+ channel antagonism on ventricular arrhythmogenesis in murine hearts containing a modification in the Scn5a gene modelling human long QT syndrome 3.
作者信息
Thomas Glyn, Gurung Iman S, Killeen Matthew J, Hakim Parvez, Goddard Catharine A, Mahaut-Smith Martyn P, Colledge William H, Grace Andrew A, Huang Christopher L-H
机构信息
Section of Cardiovascular Biology, Department of Biochemistry, University of Cambridge, Tennis Court Road, Cambridge CB2 1QW, UK.
出版信息
J Physiol. 2007 Jan 1;578(Pt 1):85-97. doi: 10.1113/jphysiol.2006.121921. Epub 2006 Nov 16.
Ventricular arrhythmogenesis in long QT 3 syndrome (LQT3) involves both triggered activity and re-entrant excitation arising from delayed ventricular repolarization. Effects of specific L-type Ca2+ channel antagonism were explored in a gain-of-function murine LQT3 model produced by a DeltaKPQ 1505-1507 deletion in the SCN5A gene. Monophasic action potentials (MAPs) were recorded from epicardial and endocardial surfaces of intact, Langendorff-perfused Scn5a+/Delta hearts. In untreated Scn5a+/Delta hearts, epicardial action potential duration at 90% repolarization (APD90) was 60.0 +/- 0.9 ms compared with 46.9 +/- 1.6 ms in untreated wild-type (WT) hearts (P < 0.05; n = 5). The corresponding endocardial APD(90) values were 52.0 +/- 0.7 ms and 53.7 +/- 1.6 ms in Scn5a+/Delta and WT hearts, respectively (P > 0.05; n = 5). Epicardial early afterdepolarizations (EADs), often accompanied by spontaneous ventricular tachycardia (VT), occurred in 100% of MAPs from Scn5a+/Delta but not in any WT hearts (n = 10). However, EAD occurrence was reduced to 62 +/- 7.1%, 44 +/- 9.7%, 10 +/- 10% and 0% of MAPs following perfusion with 10 nm, 100 nm, 300 nm and 1 mum nifedipine, respectively (P < 0.05; n = 5), giving an effective IC50 concentration of 79.3 nm. Programmed electrical stimulation (PES) induced VT in all five Scn5a+/Delta hearts (n = 5) but not in any WT hearts (n = 5). However, repeat PES induced VT in 3, 2, 2 and 0 out of 5 Scn5a+/Delta hearts following perfusion with 10 nm, 100 nm, 300 nm and 1 mum nifedipine, respectively. Patch clamp studies in isolated ventricular myocytes from Scn5a+/Delta and WT hearts confirmed that nifedipine (300 nm) completely suppressed the inward Ca2+ current but had no effect on inward Na+ currents. No significant effects were seen on epicardial APD90, endocardial APD90 or ventricular effective refractory period in Scn5a+/Delta and WT hearts following perfusion with nifedipine at 1 nm, 10 nm, 100 nm, 300 nm and 1 microm nifedipine concentrations. We conclude that L-type Ca2+ channel antagonism thus exerts specific anti-arrhythmic effects in Scn5a+/Delta hearts through suppression of EADs.
长QT3综合征(LQT3)的室性心律失常机制涉及触发活动和由心室复极延迟引起的折返激动。我们在由SCN5A基因的DeltaKPQ 1505 - 1507缺失产生的功能获得性小鼠LQT3模型中探究了特异性L型Ca2+通道拮抗作用的影响。从完整的、Langendorff灌注的Scn5a+/Delta心脏的心外膜和心内膜表面记录单相动作电位(MAP)。在未处理的Scn5a+/Delta心脏中,90%复极时的心外膜动作电位时程(APD90)为60.0±0.9毫秒,而未处理的野生型(WT)心脏为46.9±1.6毫秒(P<0.05;n = 5)。Scn5a+/Delta和WT心脏中相应的心内膜APD90值分别为52.0±0.7毫秒和53.7±1.6毫秒(P>0.05;n = 5)。心外膜早期后除极(EAD)常伴有自发性室性心动过速(VT),在Scn5a+/Delta心脏的100%的MAP中出现,而在任何WT心脏中均未出现(n = 10)。然而,在用10 nM、100 nM、300 nM和1 μM硝苯地平灌注后,EAD的发生率分别降至MAP的62±7.1%、44±9.7%、10±10%和0%(P<0.05;n = 5),有效IC50浓度为79.3 nM。程序电刺激(PES)在所有五只Scn5a+/Delta心脏中诱发出VT(n = 5),而在任何WT心脏中均未诱发出VT(n = 5)。然而,在用10 nM、100 nM、300 nM和1 μM硝苯地平灌注后,五只Scn5a+/Delta心脏中分别有3只、2只、2只和0只在重复PES时诱发出VT。对来自Scn5a+/Delta和WT心脏的分离心室肌细胞进行的膜片钳研究证实,硝苯地平(300 nM)完全抑制内向Ca2+电流,但对内向Na+电流无影响。在用1 nM、10 nM、100 nM、300 nM和1 μM硝苯地平浓度灌注后,Scn5a+/Delta和WT心脏的心外膜APD90、心内膜APD90或心室有效不应期均未观察到显著影响。我们得出结论,L型Ca2+通道拮抗作用通过抑制EADs从而在Scn5a+/Delta心脏中发挥特异性抗心律失常作用。
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