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氟西汀:多个固定剂量下的激活和镇静作用。

Fluoxetine: activating and sedating effects at multiple fixed doses.

作者信息

Beasley C M, Sayler M E, Weiss A M, Potvin J H

机构信息

Lilly Research Laboratories, Eli Lilly and Company, Indianapolis, IN 46285.

出版信息

J Clin Psychopharmacol. 1992 Oct;12(5):328-33.

PMID:1479050
Abstract

Serotonin uptake inhibitors are generally considered activating antidepressants. To assess rates and temporal patterns of activation and sedation as well as dose-effect relationships, adverse event data were evaluated from a fixed-dose study comparing placebo and fluoxetine 5, 20, and 40 mg/day in the treatment of major depressive disorder (N = 363) and two fixed-dose studies pooled together comparing placebo and fluoxetine 20, 40, and 60 mg/day in the treatment of major depressive disorder (N = 746). The adverse events nervousness, anxiety, agitation, and insomnia were considered indicative of activation; somnolence and asthenia were considered indicative of sedation. Activation and sedation were both statistically significant (p less than or equal to 0.05) treatment-emergent phenomena, but dose-effect relationships differed. Activation rates were relatively stable between 5 and 40 mg/day, and then increased at 60 mg/day. Sedation rates increased linearly to 40 mg/day and then were comparable at 40 and 60 mg/day. Discontinuations for either phenomenon were uncommon. The temporal patterns of first occurrences and persistence of activation and sedation differed. First occurrences of activation peaked early and declined over time with all doses. First occurrences of sedation also peaked early with all doses, but there may have been greater variability in first occurrences of sedation over time with lower doses. Persistent occurrences of sedation may decline less over time than persistent occurrences of activation.

摘要

血清素摄取抑制剂通常被认为是具有激活作用的抗抑郁药。为了评估激活和镇静的发生率及时间模式以及剂量效应关系,我们从一项固定剂量研究中评估了不良事件数据,该研究比较了安慰剂与氟西汀5、20和40毫克/天治疗重度抑郁症(N = 363)的效果,还评估了两项合并的固定剂量研究,这两项研究比较了安慰剂与氟西汀20、40和60毫克/天治疗重度抑郁症(N = 746)的效果。不良事件如紧张、焦虑、激动和失眠被视为激活的指标;嗜睡和乏力被视为镇静的指标。激活和镇静都是具有统计学意义(p小于或等于0.05)的治疗中出现的现象,但剂量效应关系有所不同。激活率在5至40毫克/天之间相对稳定,然后在60毫克/天时增加。镇静率线性增加至40毫克/天,然后在40和60毫克/天时相当。因这两种现象而停药的情况并不常见。激活和镇静首次出现及持续存在的时间模式有所不同。激活的首次出现早期达到峰值,然后随所有剂量随时间下降。镇静的首次出现也在所有剂量下早期达到峰值,但较低剂量下镇静首次出现随时间的变异性可能更大。与持续性激活相比,持续性镇静随时间的下降可能较少。

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