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Timing of pediatric intensive care risk assessment: Does it matter*

机译:儿科重症监护风险评估的时机:是否重要*

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Background: Major depressive disorder is a prevalent and disabling illness. Notwithstanding numerous advances in the pharmacological treatment of depression, approximately 70% of patients do not remit after first-line antidepressant treatment. Methods: The MEDLINE/PubMed, EMBASE and ClinicalTrials.gov electronic databases were searched from inception to October 1, 2013, for randomized controlled trials (RCT), relevant open-label trials, meta-analyses and ongoing trials of pharmacological and psychotherapeutic approaches to treatment-resistant depression (TRD). Results: Switching to a different antidepressant is a useful option following nonresponse to a first-line agent. Although widely used in clinical practice, there is limited evidence to support antidepressant combination for TRD. Notwithstanding evidence for lithium or T3 augmentation to be successful in TRD, most studies were carried out when participants were treated with tricyclic antidepressants (TCA). Of the available strategies to augment the response to new-generation antidepressants, the use of some atypical antipsychotics is best supported by evidence. Several novel therapeutic options are currently discussed. Evidence suggests that cognitive therapy (CT) is an effective strategy for TRD. Conclusions: The success of switching to a different antidepressant following a first-line agent is supported by evidence, but there is limited evidence for effective combination strategies. Lithium and T3 augmentation of TCA have the strongest evidence base for successful treatment of TRD. The use of augmentation of newer-generation antidepressants with atypical antipsychotics is supported by a growing evidence base. Current evidence supports CT as an effective strategy for TRD. There is a need for additional large-scale RCT of TRD. The development of new antidepressants targeting novel pathways opens a promising perspective for the management of TRD.
机译:背景:重度抑郁症是一种普遍且致残的疾病。尽管抑郁症的药理治疗取得了许多进展,但一线抗抑郁药治疗后约有70%的患者无法缓解。方法:从开始到2013年10月1日,搜索MEDLINE / PubMed,EMBASE和ClinicalTrials.gov电子数据库,以进行随机对照试验(RCT),相关的开放标签试验,荟萃分析以及正在进行中的药理学和心理治疗方法试验抗治疗性抑郁症(TRD)。结果:在对一线药物无反应后,改用其他抗抑郁药是一个有用的选择。尽管在临床实践中被广泛使用,但仅有有限的证据支持抗抑郁药可用于TRD。尽管有证据表明锂或T3增强在TRD中是成功的,但大多数研究是在接受三环抗抑郁药(TCA)治疗的受试者中进行的。在增加对新一代抗抑郁药反应的可用策略中,使用某些非典型抗精神病药最好得到证据的支持。当前讨论了几种新颖的治疗选择。有证据表明,认知疗法(TR)是一种有效的TRD策略。结论:一线药物后成功转向另一种抗抑郁药的证据有力,但有效联合策略的证据有限。 TCA的锂和T3增强是成功治疗TRD的最强有力的证据基础。越来越多的证据支持使用非典型抗精神病药增强新一代抗抑郁药的使用。当前证据支持CT作为TRD的有效策略。需要额外的TRD大规模RCT。针对新型途径的新型抗抑郁药的开发为TRD的管理打开了广阔的前景。

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