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雷美替胺(8 毫克)、佐匹克隆(7.5 毫克)和安慰剂对健康成年受试者次日高速公路驾驶表现、记忆功能、精神运动表现和情绪的影响。

Next-day effects of ramelteon (8 mg), zopiclone (7.5 mg), and placebo on highway driving performance, memory functioning, psychomotor performance, and mood in healthy adult subjects.

机构信息

Utrecht University, Utrecht Institute for Pharmaceutical Sciences, Division of Pharmacology, Utrecht, The Netherlands.

出版信息

Sleep. 2011 Oct 1;34(10):1327-34. doi: 10.5665/SLEEP.1272.

Abstract

STUDY OBJECTIVES

To evaluate the next-morning residual effects of ramelteon (8 mg), zopiclone (7.5 mg), and placebo on driving performance, memory functioning, psychomotor performance, and mood in healthy adult subjects following bedtime dosing and a middle of the night awakening.

DESIGN

Single-center, randomized, double-blind, double-dummy, placebo-controlled, crossover study.

SETTING

Utrecht University, The Netherlands.

PARTICIPANTS

30 healthy volunteers (15 males and 15 females).

INTERVENTIONS

a single dose of ramelteon (8 mg), zopiclone (7.5 mg), and placebo, administered at bedtime.

MEASUREMENTS

A balance test was performed at night. Other tests were performed the following morning, 8.5 h after administration. Subjects performed a 100-km highway driving test in normal traffic. Primary outcome measure was the standard deviation of the lateral position (SDLP), i.e., the weaving of the car. After driving, cognitive, memory, and psychomotor tests were performed and mood was assessed.

RESULTS

SDLP was significantly increased after the intake of ramelteon (+2.2 cm) and zopiclone (+2.9 cm). Ramelteon and zopiclone produced significant impairment on reaction time (P<0.024) in the Sternberg Memory Scanning Test, slow (P<0.007) and fast (P<0.010) tracking, reaction speed (P<0.015) and tracking (P<0.001) in the Divided Attention Test, and delayed recall (P<0.032) in the Word Learning Test. In contrast to ramelteon, zopiclone additionally impaired performance on the Digit Symbol Substitution Test (P<0.001) and the balance test (P<0.001).

CONCLUSIONS

Ramelteon (8 mg) and zopiclone (7.5 mg) significantly impaired driving performance, cognitive, memory, and psychomotor performance the morning following bedtime administration. In contrast to zopiclone, ramelteon produced no balance impairments. CLINICAL TRIAL IDENTIFIER: NCT00319215 (www.clinicaltrials.gov).

摘要

研究目的

评估雷美替胺(8 毫克)、佐匹克隆(7.5 毫克)和安慰剂在下床后和半夜醒来时对健康成年受试者次日早晨残留效应的影响,包括驾驶表现、记忆功能、精神运动表现和情绪。

设计

单中心、随机、双盲、双模拟、安慰剂对照、交叉研究。

地点

荷兰乌得勒支大学。

参与者

30 名健康志愿者(15 名男性和 15 名女性)。

干预措施

睡前单次服用雷美替胺(8 毫克)、佐匹克隆(7.5 毫克)和安慰剂。

测量

夜间进行平衡测试。其他测试在给药后 8.5 小时的次日早晨进行。受试者在正常交通中进行 100 公里高速公路驾驶测试。主要测量指标是侧向位置标准差(SDLP),即汽车的编织。驾驶后,进行认知、记忆和精神运动测试,并评估情绪。

结果

雷美替胺(+2.2 厘米)和佐匹克隆(+2.9 厘米)摄入后 SDLP 显著增加。雷美替胺和佐匹克隆显著影响斯特恩伯格记忆扫描测试中的反应时间(P<0.024),在 Sternberg 记忆扫描测试中,显著影响慢(P<0.007)和快(P<0.010)跟踪、反应速度(P<0.015)和跟踪(P<0.001)在分散注意测试中,以及延迟回忆(P<0.032)在单词学习测试中。与雷美替胺不同,佐匹克隆还显著影响数字符号替代测试(P<0.001)和平衡测试(P<0.001)的表现。

结论

雷美替胺(8 毫克)和佐匹克隆(7.5 毫克)在下床后给药次日早晨显著影响驾驶表现、认知、记忆和精神运动表现。与佐匹克隆不同,雷美替胺不会产生平衡损伤。

临床试验标识符

NCT00319215(www.clinicaltrials.gov)。

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