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替加宾治疗第一晚的睡眠效应可预测创伤后应激障碍在 3 周时的反应。

The sleep effects of tiagabine on the first night of treatment predict post-traumatic stress disorder response at three weeks.

机构信息

1Department of Psychiatry and Behavioral Sciences, Duke University Medical Center, Durham, NC, USA.

出版信息

J Psychopharmacol. 2014 May;28(5):457-65. doi: 10.1177/0269881113509903. Epub 2013 Nov 28.

Abstract

INTRODUCTION

We sought to test the hypothesis that improvements in sleep might mediate treatment-related improvements in daytime symptoms of post-traumatic stress disorder (PTSD). We evaluated whether changes in sleep occurring on the first night of tiagabine (a gamma-amino butyric acid (GABA) reuptake inhibitor) administration predicted subsequent PTSD response.

METHODS

This was an open-label three-week polysomnographic (PSG) study of nightly treatment with tiagabine dosing from 2-12 mg including 20 adults with PTSD with ≥30 min of self-reported and PSG wake time after sleep onset (WASO).

RESULTS

A treatment night 1 decrease in self-reported and PSG WASO and an increase in slow-wave sleep (SWS) accounted for 94% of the variance in week 3 Short PTSD Rating Interview (SPRINT) score, the primary outcome measure (p<0.001). Increased night 1 SWS also accounted for 91% of the variance in Work/School Impairment and 45% of the variance in Social Life Impairment as measured with the Sheehan Disability Scale (p<0.001). These relationships were much stronger correlates of three-week outcome than three-week sleep effects.

CONCLUSIONS

The initial sleep response to tiagabine may mediate or be an indicator of the subsequent PTSD response. The findings highlight the importance of sleep maintenance and SWS in the treatment of PTSD and also suggest a potential relationship between SWS and daytime function.

摘要

简介

我们试图验证以下假说,即睡眠的改善可能介导创伤后应激障碍(PTSD)日间症状的治疗相关改善。我们评估了加巴喷丁(一种γ-氨基丁酸(GABA)再摄取抑制剂)给药的第一个晚上发生的睡眠变化是否可以预测随后的 PTSD 反应。

方法

这是一项为期三周的开放性标签多导睡眠图(PSG)研究,每晚使用加巴喷丁治疗,剂量为 2-12mg,包括 20 名 PTSD 患者,他们有≥30 分钟的自我报告和 PSG 睡眠后觉醒时间(WASO)。

结果

治疗第 1 天的自我报告和 PSG WASO 减少,慢波睡眠(SWS)增加,这可解释第 3 周 PTSD 短期评定访谈(SPRINT)评分(主要结局指标)变化的 94%(p<0.001)。第 1 天 SWS 的增加也可解释 Sheehan 残疾量表(SDSS)评估的工作/学业障碍变化的 91%和社会生活障碍变化的 45%(p<0.001)。这些关系是三周后结果的更强相关因素,而不是三周后的睡眠影响。

结论

加巴喷丁的初始睡眠反应可能是随后 PTSD 反应的中介或指标。这些发现强调了维持睡眠和 SWS 在 PTSD 治疗中的重要性,也提示了 SWS 与日间功能之间可能存在关系。

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