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Neurobiol Learn Mem. 2014 Jul;112:204-11. doi: 10.1016/j.nlm.2013.11.018. Epub 2013 Dec 1.
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Early PTSD symptom trajectories: persistence, recovery, and response to treatment: results from the Jerusalem Trauma Outreach and Prevention Study (J-TOPS).创伤后应激障碍症状早期轨迹:持续性、恢复和治疗反应:来自耶路撒冷创伤外联和预防研究(J-TOPS)的结果。
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Epigenetic Mechanisms Shape the Biological Response to Trauma and Risk for PTSD: A Critical Review.表观遗传机制塑造对创伤的生物学反应及创伤后应激障碍风险:一项批判性综述
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The efficacy of initial hydrocortisone administration at preventing posttraumatic distress in adult trauma patients: a randomized trial.早期给予氢化可的松对预防成人创伤患者创伤后痛苦的疗效:一项随机试验。
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预防创伤后应激障碍(PTSD)的药物干预措施。

Pharmacological interventions for preventing post-traumatic stress disorder (PTSD).

作者信息

Amos Taryn, Stein Dan J, Ipser Jonathan C

机构信息

Department of Psychiatry and Mental Health, University of Cape Town, Education Centre, Valkenberg Hospital, Private Bage X1, Observatory, Cape Town, South Africa, 7925.

出版信息

Cochrane Database Syst Rev. 2014 Jul 8;2014(7):CD006239. doi: 10.1002/14651858.CD006239.pub2.

DOI:10.1002/14651858.CD006239.pub2
PMID:25001071
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11064759/
Abstract

BACKGROUND

Post-traumatic stress disorder (PTSD) is a debilitating disorder which, after a sufficient delay, may be diagnosed amongst individuals who respond with intense fear, helplessness or horror to traumatic events. There is some evidence that the use of pharmacological interventions immediately after exposure to trauma may reduce the risk of developing of PTSD.

OBJECTIVES

To assess the effects of pharmacological interventions for the prevention of PTSD in adults following exposure to a traumatic event.

SEARCH METHODS

We searched the Cochrane Depression, Anxiety and Neurosis Controlled Trials Register (CCDANCTR-Studies and CCDANCTR-References) (to 14 February 2014). This register contains relevant reports of randomised controlled trials from the following bibliographic databases: CENTRAL (all years); EMBASE (1974 to date); MEDLINE (1950 to date) and PsycINFO (1967 to date). We identified unpublished trials by searching the National Institute of Health (NIH) Reporter, the metaRegister of Controlled Trials database (mRCT) and the WHO International Clinical Trials Registry Platform (to December 2013). We scanned the reference lists of articles for additional studies. We placed no constraints on language and setting.

SELECTION CRITERIA

We restricted studies to randomised controlled trials (RCTs) of pharmacological interventions compared with placebo for the prevention of PTSD in adults.

DATA COLLECTION AND ANALYSIS

Two authors (TA and JI) independently assessed trials for eligibility and inclusion based on the review selection criteria. We independently extracted sample, methodological, outcome and 'Risk of bias' data, as well as the number of side effects, from each trial and entered these into a customised data extraction form. We contacted investigators for missing information. We calculated summary statistics for continuous and dichotomous variables (if provided). We did not undertake subgroup analyses due to the small number of included studies.

MAIN RESULTS

We included nine short-term RCTs (duration 12 weeks or less) in the analysis (345 participants; age range 18 to 76 years). Participants were exposed to a variety of traumas, ranging from assault, traffic accidents and work accidents to cardiac surgery and septic shock. Seven studies were conducted at single centres. The seven RCTs included four hydrocortisone studies, three propranolol studies (of which one study had a third arm investigating gabapentin), and single trials of escitalopram and temazepam. Outcome assessment measures included the Clinician-Administered PTSD Scale (CAPS), the 36-Item Short-Form Health Survey (SF-36) and the Center for Epidemiological Studies - Depression Scale (CES-D).In four trials with 165 participants there was moderate quality evidence for the efficacy of hydrocortisone in preventing the onset of PTSD (risk ratio (RR) 0.17; 95% confidence interval (CI) 0.05 to 0.56; P value = 0.004), indicating that between seven and 13 patients would need to be treated with this agent in order to prevent the onset of PTSD in one patient. There was low quality evidence for preventing the onset of PTSD in three trials with 118 participants treated with propranolol (RR 0.62; 95% CI 0.24 to 1.59; P value = 0.32). Drop-outs due to treatment-emergent side effects, where reported, were low for all of the agents tested. Three of the four RCTs of hydrocortisone reported that medication was more effective than placebo in reducing PTSD symptoms after a median of 4.5 months after the event. None of the single trials of escitalopram, temazepam and gabapentin demonstrated evidence that medication was superior to placebo in preventing the onset of PTSD.Seven of the included RCTs were at a high risk of bias. Differential drop-outs between groups undermined the results of three studies, while one study failed to describe how the allocation of medication was concealed. Other forms of bias that might have influenced study results included possible confounding through group differences in concurrent medication and termination of the study based on treatment response.

AUTHORS' CONCLUSIONS: There is moderate quality evidence for the efficacy of hydrocortisone for the prevention of PTSD development in adults. We found no evidence to support the efficacy of propranolol, escitalopram, temazepam and gabapentin in preventing PTSD onset. The findings, however, are based on a few small studies with multiple limitations. Further research is necessary in order to determine the efficacy of pharmacotherapy in preventing PTSD and to identify potential moderators of treatment effect.

摘要

背景

创伤后应激障碍(PTSD)是一种使人衰弱的疾病,在经过足够长的延迟期后,可在那些对创伤事件表现出强烈恐惧、无助或惊恐的个体中被诊断出来。有证据表明,在遭受创伤后立即使用药物干预可能会降低患创伤后应激障碍的风险。

目的

评估药物干预对预防成年人创伤事件后创伤后应激障碍的效果。

检索方法

我们检索了Cochrane抑郁、焦虑与神经症对照试验注册库(CCDANCTR-研究和CCDANCTR-参考文献)(截至2014年2月14日)。该注册库包含来自以下书目数据库的随机对照试验的相关报告:Cochrane系统评价数据库(CENTRAL)(所有年份);EMBASE(1974年至今);MEDLINE(1950年至今)和PsycINFO(1967年至今)。我们通过检索美国国立卫生研究院(NIH)报告、对照试验元注册数据库(mRCT)和世界卫生组织国际临床试验注册平台(截至2013年12月)来识别未发表的试验。我们浏览文章的参考文献列表以寻找其他研究。我们对语言和研究背景没有限制。

选择标准

我们将研究限制为针对成年人预防创伤后应激障碍的药物干预与安慰剂对比的随机对照试验(RCT)。

数据收集与分析

两位作者(TA和JI)根据综述选择标准独立评估试验是否符合资格及是否纳入。我们独立从每个试验中提取样本、方法学、结局和“偏倚风险”数据,以及副作用数量,并将这些数据录入定制的数据提取表格。我们联系研究者获取缺失信息。我们计算了连续变量和二分变量的汇总统计量(如果提供了这些数据)。由于纳入研究数量较少,我们未进行亚组分析。

主要结果

我们纳入了9项短期随机对照试验(持续时间为12周或更短)进行分析(345名参与者;年龄范围18至76岁)。参与者经历了各种创伤,从袭击、交通事故和工伤事故到心脏手术和感染性休克。7项研究在单一中心进行。这7项随机对照试验包括4项氢化可的松研究、3项普萘洛尔研究(其中1项研究有第三个研究组调查加巴喷丁),以及艾司西酞普兰和替马西泮的单项试验。结局评估指标包括临床医生评定的创伤后应激障碍量表(CAPS)、36项简明健康调查量表(SF-36)和流行病学研究中心抑郁量表(CES-D)。在4项涉及165名参与者的试验中,有中等质量证据表明氢化可的松在预防创伤后应激障碍发作方面有效(风险比(RR)0.17;95%置信区间(CI)0.05至0.56;P值 = 0.004),这表明为预防1例创伤后应激障碍发作,需要用该药物治疗7至13名患者。在3项涉及118名接受普萘洛尔治疗参与者的试验中,有低质量证据表明预防创伤后应激障碍发作有效(RR 0.62;95% CI 0.24至1.59;P值 = 0.32)。在所测试的所有药物中,因治疗中出现的副作用导致的退出率据报告都较低。4项氢化可的松随机对照试验中的3项报告称,在事件发生后中位4.5个月时,药物在减轻创伤后应激障碍症状方面比安慰剂更有效。艾司西酞普兰、替马西泮和加巴喷丁的单项试验均未显示药物在预防创伤后应激障碍发作方面优于安慰剂的证据。纳入的随机对照试验中有7项存在高偏倚风险。组间差异退出影响了3项研究的结果,而1项研究未描述药物分配是如何隐藏的。其他可能影响研究结果的偏倚形式包括通过同时用药的组间差异可能造成的混杂,以及基于治疗反应终止研究。

作者结论

有中等质量证据表明氢化可的松对预防成年人创伤后应激障碍的发生有效。我们没有发现证据支持普萘洛尔、艾司西酞普兰、替马西泮和加巴喷丁在预防创伤后应激障碍发作方面的有效性。然而,这些发现基于一些有多种局限性的小型研究。有必要进行进一步研究以确定药物疗法在预防创伤后应激障碍方面的有效性,并确定治疗效果的潜在调节因素。