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三唑仑和劳拉西泮对人类学习、表现及受试者评分的急性影响。

Acute effects of triazolam and lorazepam on human learning, performance and subject ratings.

作者信息

Rush C R, Higgins S T, Bickel W K, Hughes J R

机构信息

Department of Psychiatry, University of Vermont, Burlington.

出版信息

J Pharmacol Exp Ther. 1993 Mar;264(3):1218-26.

PMID:8450459
Abstract

Triazolam (0,0.125, 0.25, 0.5, and 0.75 mg/70 kg) and lorazepam (0, 1, 2, 4 and 6 mg/70 kg) were compared in eight healthy men by using a double-blind, crossover design. Triazolam was chosen for study to examine experimentally whether it produces greater behavioral impairment than other benzodiazepines as reported previously. Lorazepam was chosen as the comparison drug because of its well documented behavioral effects and because it has a short metabolic half-life and no active metabolite, which eliminates the possible confounding effects of drug accumulation. Drug effects were assessed before and every 30 min for 8 hr after drug administration. Learning was chosen for study because it is a fundamental component of more complex behavioral processes such as recall, and benzodiazepines are known to disrupt learning. A psychomotor task and subject-rating scales, assessing drug effects and abuse potential, were also included to provide a more comprehensive comparison of these compounds. Triazolam and lorazepam dose-dependently disrupted learning and psychomotor performance and increased subject ratings of sedation to a comparable degree. These findings do not support allegations that triazolam produces greater behavioral impairment than other commonly used benzodiazepines.

摘要

采用双盲交叉设计,对8名健康男性受试者比较了三唑仑(0、0.125、0.25、0.5和0.75mg/70kg)和劳拉西泮(0、1、2、4和6mg/70kg)的效果。选择三唑仑进行研究,以通过实验检验它是否如先前报道的那样比其他苯二氮䓬类药物产生更大的行为损害。选择劳拉西泮作为对照药物,是因为其行为效应已有充分记录,且其代谢半衰期短且无活性代谢产物,可消除药物蓄积可能产生的混杂效应。在给药前及给药后8小时内,每30分钟评估一次药物效果。选择学习作为研究对象,是因为它是回忆等更复杂行为过程的基本组成部分,且已知苯二氮䓬类药物会干扰学习。还纳入了一项精神运动任务和受试者评分量表,以评估药物效果和滥用潜力,从而对这些化合物进行更全面的比较。三唑仑和劳拉西泮均剂量依赖性地干扰学习和精神运动表现,并在相当程度上提高了受试者的镇静评分。这些发现不支持关于三唑仑比其他常用苯二氮䓬类药物产生更大行为损害的说法。

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