Donoghue S, Payne P N, Allan G
J Cardiovasc Pharmacol. 1987 Jan;9(1):12-8.
The frequency, use, and voltage-dependence of the effects of a novel antiarrhythmic agent, BW A256C, on the maximum rate of depolarization (Vmax) of action potentials in guinea-pig right ventricle were studied using standard microelectrode recording techniques in vitro. BW A256C (10(-6) M) reduced Vmax in a frequency-dependent way in the range 0.33-3.3 Hz; the maximum reduction was at the highest frequency. BW A256C did not cause resting block of Vmax. The onset of use-dependent Vmax reduction at 3.3 Hz followed a monoexponential function with a very slow rate constant, 0.019 +/- 0.003 AP-1. The recovery from use-dependent reduction, studied by applying single extra stimuli at various times after trains of stimuli at 3.3 Hz, was also very slow; half-life (t 1/2) for recovery was 119.0 +/- 19.2 s, and the time constant tre was 171.7 +/- 27.7 s. For comparison, the values for Flecainide (10(-5) M), obtained under identical conditions, were: rateon, 0.106 +/- 0.010 AP-1; t 1/2, 7.68 +/- 0.20 s; tre 11.07 +/- 0.29 s (means +/- SEM). In the presence of BW A256C (10(-6) M), the normalised diastolic membrane potential-Vmax curve was significantly shifted in the hyperpolarizing direction. The mean shift was 5.5 +/- 1.1 mV, measured at the 50% reduction of Vmax level. BW A256C is therefore classified as a novel "slow" class 1C antiarrhythmic agent.
采用标准微电极体外记录技术,研究了新型抗心律失常药物BW A256C对豚鼠右心室动作电位最大去极化速率(Vmax)的作用频率、用途及电压依赖性。BW A256C(10^(-6)M)在0.33 - 3.3Hz范围内以频率依赖性方式降低Vmax;最大降幅出现在最高频率时。BW A256C不会导致Vmax的静息阻滞。在3.3Hz时,使用依赖性Vmax降低的起始遵循单指数函数,速率常数非常缓慢,为0.019±0.003 AP^(-1)。通过在3.3Hz的刺激序列后不同时间施加单个额外刺激来研究使用依赖性降低后的恢复情况,恢复也非常缓慢;恢复的半衰期(t1/2)为119.0±19.2秒,时间常数tre为171.7±27.7秒。作为比较,在相同条件下获得的氟卡尼(10^(-5)M)的值为:rateon,0.106±0.010 AP^(-1);t1/2,7.68±0.20秒;tre 11.07±0.29秒(平均值±标准误)。在BW A256C(10^(-6)M)存在的情况下,正常化的舒张期膜电位 - Vmax曲线在超极化方向上显著偏移。在Vmax水平降低50%时测量,平均偏移为5.5±1.1 mV。因此,BW A256C被归类为一种新型的“慢”1C类抗心律失常药物。
