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首页> 外文期刊>CNS neuroscience & therapeutics. >Effect of Acute Posttrauma Propranolol on PTSD Outcome and Physiological Responses During Script‐Driven Imagery
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Effect of Acute Posttrauma Propranolol on PTSD Outcome and Physiological Responses During Script‐Driven Imagery

机译:脚本驱动影像过程中急性创伤后普萘洛尔对PTSD结果和生理反应的影响

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SUMMARY Introduction: Animal and human research suggests that the development of posttraumatic stress disorder (PTSD) may involve the overconsolidation of memories of a traumatic experience. Previous studies have attempted to use pharmaceutical agents, especially the β‐adrenergic blocker propranolol, to reduce this overconsolidation. Aims: In this randomized, placebo‐controlled study of the efficacy of propranolol in reducing the development of PTSD, we optimized dosages and conducted both psychophysiological and clinical assessments 1 and 3 months after the traumatic event. Forty‐one emergency department patients who had experienced a qualifying acute psychological trauma were randomized to receive up to 240 mg/day of propranolol or placebo for 19 days. At 4 and 12 weeks post‐trauma, PTSD symptoms were assessed. One week later, participants engaged in script‐driven imagery of their traumatic event while psychophysiological responses were measured. Results: Physiological reactivity during script‐driven traumatic imagery, severity of PTSD symptoms, and the rate of the PTSD diagnostic outcome were not significantly different between the two groups. However, post hoc subgroup analyses showed that in participants with high drug adherence, at the 5‐week posttrauma assessment, physiological reactivity was significantly lower during script‐driven imagery in the propranolol than in the placebo subjects. Conclusions: The physiological results provide some limited support for a model of PTSD in which a traumatic conditioned response is reduced by posttrauma propranolol. However, the clinical results from this study do not support the preventive use of propranolol in the acute aftermath of a traumatic event.
机译:简介简介:动物和人类研究表明,创伤后应激障碍(PTSD)的发展可能涉及创伤经历记忆的过度巩固。先前的研究尝试使用药物,尤其是β-肾上腺素能阻断剂普萘洛尔,以减少这种过度合并。目的:在这项关于普萘洛尔减少PTSD发生的功效的随机,安慰剂对照研究中,我们优化了剂量,并在创伤事件发生后1和3个月进行了心理生理和临床评估。随机将经历过适当的急性心理创伤的41名急诊科患者接受19天每天240毫克的心得安或安慰剂治疗。创伤后4周和12周,评估了PTSD症状。一周后,参与者测量了他们的创伤事件的脚本驱动图像,同时测量了心理生理反应。结果:两组在脚本驱动的创伤性影像学中的生理反应性,PTSD症状的严重程度以及PTSD诊断结果的发生率无显着差异。但是,事后亚组分析显示,在药物依从性较高的参与者中,在创伤后5周评估中,普萘洛尔在脚本驱动的影像学过程中的生理反应性显着低于安慰剂受试者。结论:生理结果为创伤后普萘洛尔减轻创伤性条件性反应的创伤后应激障碍模型提供了有限的支持。但是,这项研究的临床结果不支持在创伤事件的急性后果中预防性使用普萘洛尔。

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