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Pharmacological prevention and early treatment of post-traumatic stress disorder and acute stress disorder: a systematic review and meta-analysis

机译:药理预防和早期治疗后创伤后应激障碍和急性应激障碍:系统审查和荟萃分析

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Post-traumatic stress disorder (PTSD) is a common mental disorder associated with significant distress and reduced functioning. Its occurrence after a severe traumatic event and association with characteristic neurobiological changes make PTSD a good candidate for pharmacological prevention and early treatment. The primary aim for this systematic review and meta-analysis was to assess whether pharmacological interventions when compared to placebo, or other pharmacological/psychosocial interventions resulted in a clinically significant reduction or prevention of symptoms, improved functioning or quality of life, presence of disorder, or adverse effects. A systematic search was undertaken to identify RCTs, which used early pharmacotherapy (within three months of a traumatic event) to prevent and treat PTSD and acute stress disorder (ASD) in children and adults. Using Cochrane Collaboration methodology, RCTs were identified and rated for risk of bias. Available data was pooled to calculate risk ratios (RR) for PTSD prevalence and standardised mean differences (SMD) for PTSD severity. 19 RCTs met the inclusion criteria; 16 studies with adult participants and three with children. The methodological quality of most trials was low. Only hydrocortisone in adults was found to be superior to placebo (3 studies, n?=?88, RR: 0.21 (CI 0.05 to 0.89)) although this was in populations with severe physical illness, raising concerns about generalisability. No significant effects were found for the other pharmacotherapies investigated (propranolol, oxytocin, gabapentin, fish oil (1470?mg DHA/147?mg EPA), fish oil (224?mg DHA/22.4?mg EPA), dexamethasone, escitalopram, imipramine and chloral hydrate). Hydrocortisone shows the most promise, of pharmacotherapies subjected to RCTs, as an emerging intervention in the prevention of PTSD within three months after trauma and should be a target for further investigation. The limited evidence for hydrocortisone and its adverse effects mean it cannot be recommended for routine use, but, it could be considered as a preventative intervention for people with severe physical illness or injury, shortly after a traumatic event, as long as there are no contraindications. More research is needed using larger, high quality RCTs to establish the most efficacious use of hydrocortisone in different populations and optimal dosing, dosing window and route. There is currently a lack of evidence to suggest that other pharmacological agents are likely to be effective.
机译:创伤后应激障碍(PTSD)是一种常见的精神障碍,其与显着痛苦和功能降低相关。它在严重的创伤事件和与特征神经生物学变化结合后发生的发生使PTSD成为药理预防和早期治疗的良好候选者。该系统审查和荟萃分析的主要目标是评估与安慰剂相比的药理干预,或其他药理/心理社会干预措施导致临床显着减少或预防症状,改善功能或生活质量,紊乱的存在,或不利影响。进行了系统检索以鉴定rcts,其中使用早期药物治疗(在创伤事件的三个​​月内),以预防和治疗儿童和成人的急性应激障碍(ASD)。使用Cochrane协作方法,确定并评定了偏倚风险的RCT。汇集可用数据以计算可应诊性患病率的风险比(RR)和可应诊严重程度的标准化平均差异(SMD)。 19 RCT符合纳入标准; 16名与成人参与者和3名与儿童的研究。大多数试验的方法论质量很低。只发现成人中的氢化胞蔻体优于安慰剂(3项研究,N?= 88,RR:0.21(CI 0.05至0.89)),但这是具有严重身体疾病的群体,提高了对长期性的担忧。对所研究的其他药察加(ProPranolol,催产素,加巴峰,鱼油(1470×Mg DHA / 147?Mg EPA),鱼油(224?Mg DHA / 22.4?Mg EPA),Dexamethasone,Esca里普拉姆,氨基甲胺和水合物)。氢化可源性显示出对RCT的药物治疗最高的承诺,作为在创伤后三个月内预防PTSD的新兴干预,并且应该是进一步调查的目标。氢化体的有限证据及其不良反应意味着它不能推荐用于常规用途,但是,只要没有禁忌症,它可能被视为严重的身体疾病或伤害的预防干预。 。需要更多的研究使用较大,高质量的RCT,以确定不同群体和最佳给药,给药窗口和途径的氢化胞苷的最有效使用。目前缺乏证据表明其他药理学药物可能是有效的。

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