Residual Effects of Middle-of-the-Night Administration of Zaleplon and Zolpidem on Driving Ability, Memory Functions, and Psychomotor Performance

唑吡坦 数字符号替换试验 交叉研究 精神运动学习 驾驶考试 安慰剂 麻醉 听力学 催眠药 毒物控制 心理学 医学 药理学 精神科 失眠症 内科学 认知 医疗急救 病理 逻辑回归 替代医学
作者
Joris C. Verster,Edmund R. Volkerts,A.H.C.M.L. Schreuder,Erik J. E. Eijken,Janet H. G. van Heuckelum,Dieuwke S. Veldhuijzen,Marinus N. Verbaten,Isabelle Paty,Mona Darwish,Philippe Danjou,Alain Patat
出处
期刊:Journal of Clinical Psychopharmacology [Ovid Technologies (Wolters Kluwer)]
卷期号:22 (6): 576-583 被引量:178
标识
DOI:10.1097/00004714-200212000-00007
摘要

Thirty healthy volunteers participated in this two-part study. Part 1 was a single-blind, two-period crossover design to determine the effects of a single dose of ethanol (0.03% < BAC < 0.05%) or ethanol-placebo on driving ability, memory, and psychomotor performance. Part 2 was a double-blind, five-period crossover design to measure the effects of a middle-of-the-night administration of zaleplon 10 or 20 mg, zolpidem 10 or 20 mg, or placebo on driving ability 4 hours after administration and memory and psychomotor performance 6 hours after administration. The on-the-road driving test consisted of operating an instrumented automobile over a 100-km highway circuit at a constant speed (95 km/h) while maintaining a steady lateral position between the right lane boundaries. The standard deviation of lateral position (SDLP) was the primary performance parameter of the driving test. The psychomotor and memory test battery consisted of the Word Learning Test, the Critical Tracking Test, the Divided Attention Test, and the Digit Symbol Substitution Test. Data for each part were analyzed separately using ANOVA for crossover designs. Zaleplon 10 and 20 mg did not significantly impair driving ability 4 hours after middle-of-the-night administration. Relative to placebo, after zolpidem 10 mg, SDLP was significantly elevated, but the magnitude of the difference was small and not likely to be of clinical importance. Memory and psychomotor test performance was unaffected after both doses of zaleplon and zolpidem 10 mg. In contrast, zolpidem 20 mg significantly increased SDLP and speed variability. Further, zolpidem 20 mg significantly impaired performance on all psychomotor and memory tests. Finally, driving performance, Digit Symbol Substitution Test, Divided Attention Test, and immediate and delayed free recall of the Word Learning Test were significantly impaired after ethanol. The results show that zaleplon (10 and 20 mg) is a safe hypnotic devoid of next-morning residual impairment when used in the middle of the night.
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