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急性剂量的非索非那定、异丙嗪和安慰剂对健康日本志愿者认知及精神运动功能的影响。

The effects of acute doses of fexofenadine, promethazine, and placebo on cognitive and psychomotor function in healthy Japanese volunteers.

作者信息

Ridout Fran, Hindmarch Ian

机构信息

HPRU Medical Research Centre, University of Surrey, Egerton Road, Guildford, Surrey, United Kingdom.

出版信息

Ann Allergy Asthma Immunol. 2003 Apr;90(4):404-10. doi: 10.1016/S1081-1206(10)61824-8.

Abstract

BACKGROUND

Genetic variations in cross-cultural metabolic capability may attenuate the lack of central nervous system effects of fexofenadine.

OBJECTIVE

To compare the pharmacodynamics of fexofenadine and promethazine versus placebo in Japanese volunteers.

METHODS

In this randomized, crossover, double-blind study, 24 subjects received single doses of fexofenadine 60 mg and 120 mg, promethazine 25 mg, and placebo, with a 6-day washout period between treatments. Objective measures included critical flicker fusion, choice reaction time, and a compensatory tracking task. A line analog rating scale evaluated self-rated sedation. A rapid visual information-processing task evaluated vigilance at baseline and at 2 hours.

RESULTS

Fexofenadine was not significantly different from placebo on any test at any timepoint. In contrast, promethazine impaired critical flicker fusion thresholds (F[3,63] = 5.37, P = 0.0023); increased recognition reaction time (F[3,63] = 13.63, P < 0.0001) and total reaction time (F[3,63] = 12.23, P < 0.0001) components of the choice reaction time test; reduced tracking accuracy (F[3,63] = 14.25, P < 0.0001) and increased reaction times to peripheral stimuli (F[3,63] = 9.29, P < 0.0001) in the compensatory tracking task; reduced the number of valid responses (F[3,63] = 14.86, P < 0.0001) and impaired reaction times (F[3,63] = 12.02, P < 0.0001) in the rapid visual information-processing task test; and impaired subjective ratings of sedation (F[3,63] = 7.55, P = 0.0002), compared with placebo.

CONCLUSIONS

A battery of tests sensitive to impairment by promethazine failed to show any negative cognitive or psychomotor effects with fexofenadine 60 and 120 mg. Fexofenadine is an intrinsically non-impairing antihistamine in Japanese subjects.

摘要

背景

跨文化代谢能力的基因变异可能会减弱非索非那定对中枢神经系统缺乏影响的情况。

目的

比较非索非那定和异丙嗪与安慰剂在日本志愿者中的药效学。

方法

在这项随机、交叉、双盲研究中,24名受试者接受单剂量60毫克和120毫克的非索非那定、25毫克的异丙嗪以及安慰剂治疗,治疗之间有6天的洗脱期。客观测量指标包括临界闪烁融合、选择反应时间和一项补偿跟踪任务。一条视觉类似物评分量表评估自我评定的镇静程度。一项快速视觉信息处理任务评估基线和2小时时的警觉性。

结果

在任何时间点的任何测试中,非索非那定与安慰剂均无显著差异。相比之下,与安慰剂相比,异丙嗪降低了临界闪烁融合阈值(F[3,63]=5.37,P=0.0023);增加了选择反应时间测试中的识别反应时间(F[3,63]=13.63,P<0.0001)和总反应时间(F[3,63]=12.23,P<0.0001)成分;降低了补偿跟踪任务中的跟踪准确性(F[3,63]=14.25,P<0.0001)并增加了对外周刺激的反应时间(F[3,63]=9.29,P<0.0001);在快速视觉信息处理任务测试中减少了有效反应的数量(F[3,63]=14.86,P<0.0001)并损害了反应时间(F[3,63]=12.02,P<0.0001);并损害了镇静的主观评分(F[3,63]=7.55,P=0.0002)。

结论

一系列对异丙嗪损害敏感的测试未显示60毫克和120毫克非索非那定有任何负面认知或精神运动效应。在日本受试者中,非索非那定是一种本质上无损害作用的抗组胺药。

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