Keefe D L, Peters F, Winkle R A
Am Heart J. 1982 Apr;103(4 Pt 1):511-8. doi: 10.1016/0002-8703(82)90338-6.
Lorcainide, a new antiarrhythmic drug, was given to 10 patients with frequent (greater than 1/min) premature ventricular contractions (PVCs) on a baseline 24-hour Holter monitor. Each patient received lorcainide, 100 mg twice daily, and an identical placebo, in a randomized double-blind crossover trial, with 1 week in each treatment period. Before the trial and at the end of each period, routine laboratory, clinical evaluation, 12-lead ECG's, and 24-hour ambulatory ECG recordings were performed. Trough drug plasma concentration measurements were done at the end of each treatment period. All patients had reduction in PVCs, comparing drug to placebo, averaging 82.3 +/- 19.7% (mean +/- SD, p less than 0.01 by Wilcoxin ranked sum), and there was also significant decrease in the number of ventricular pairs and runs. Levels of the major metabolite, norlorcainide, ranged from 34 to 254 ng/ml (mean 160 ng/ml) and exceeded those for lorcainide, range 6 to 169 ng/ml (mean 79 ng/ml). Prolongation of PR, QRS, and QTc intervals was evident during drug therapy, as was decrease in heart rate, but these changes were minimal. The major adverse effect noted was sleep disturbance, which was often initially severe, but improved during the week of therapy.
劳卡尼,一种新型抗心律失常药物,在24小时动态心电图监测基础上给予10例频发(大于1次/分钟)室性早搏(PVC)患者。在一项随机双盲交叉试验中,每位患者每日两次服用100毫克劳卡尼和相同的安慰剂,每个治疗期为1周。在试验前和每个治疗期结束时,进行常规实验室检查、临床评估、12导联心电图及24小时动态心电图记录。在每个治疗期结束时进行药物血浆谷浓度测量。与安慰剂相比,所有患者的室性早搏均减少,平均减少82.3±19.7%(均值±标准差,Wilcoxin秩和检验p<0.01),室性成对搏动和心动过速次数也显著减少。主要代谢产物去甲劳卡尼的浓度范围为34至254纳克/毫升(平均160纳克/毫升),超过了劳卡尼的浓度范围6至169纳克/毫升(平均79纳克/毫升)。在药物治疗期间,PR、QRS和QTc间期明显延长,心率降低,但这些变化很轻微。观察到的主要不良反应是睡眠障碍,最初通常较为严重,但在治疗一周内有所改善。
