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The pH dependence on the electrophysiological effect of lidocaine in ventricular myocardium. A computer modelling study

机译:pH值取决于利多卡因在心室心肌中的电生理作用。计算机建模研究

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Lidocaine is a class I antiarrhytmic drug that blocks the sodium channels. This drug is a tertiary amine and exists as an uncharged free amine and cationic protonated form at physiologic pH. Experimental data have shown that the rate of development and recovery of block is slowed at low pH. In this work, a mathematical model of lidocaine effects has been developed. This model has been incorporated to the Luo Rudy model of guinea pig ventricular action potential and we studied the effect of lidocaine on maximum upstroke velocity (dV/dt), action potential duration (APD), conduction velocity (CV) and effective refractory period (ERP) for different values of pH and concentrations of lidocaine. This study demonstrates that 50 μmol/L of lidocaine reduces the dV/dt 36 % and 71 % as well as the CV a 8 % and 17 % for pH 7.4 and 6.4 respectively, while the ERP was increased 1.8 % and 0.6 % for pH of 7.4 and 6.4. The APD does not change when pH was modulated.
机译:利多卡因是阻断钠通道的I类抗心律失常药物。该药物是叔胺,在生理pH下以不带电荷的游离胺和阳离子质子化形式存在。实验数据表明,在低pH值下,块的形成和恢复速率会减慢。在这项工作中,开发了利多卡因作用的数学模型。该模型已被纳入豚鼠心室动作电位的Luo Rudy模型,我们研究了利多卡因对最大上风速度(dV / dt),动作电位持续时间(APD),传导速度(CV)和有效不应期的影响( ERP)用于不同的pH值和利多卡因浓度。这项研究表明,对于pH 7.4和6.4,利多卡因50μmol/ L降低dV / dt分别为36%和71%以及CV分别为8%和17%,而pH值下的ERP分别提高了1.8%和0.6% 7.4和6.4。调节pH时,APD不变。

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