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Brexpiprazole for treatment-resistant major depressive disorder

机译:Brengiprazole用于治疗耐药症状

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Introduction:Treatment-resistant depression (TRD), seldom interchangeably referred to as 'depression inadequately responding to the standard antidepressant drug,' carries a significant burden. The atypical antipsychotics represent a popular augmentation strategy for antidepressant-resistant depression, although their efficacy/safety profiles vary across different agents and presentations of depression. Areas covered: This review appraises the evidence supporting the use of brexpiprazole augmentation for major depressive disorder (MDD) adults showing an inadequate response to standard antidepressants, covering the related regulatory affairs, and essential pharmacology. Expert opinion: Brexpiprazole is a 'third-generation' antipsychotic featuring dopaminergic D-2 and serotonergic 5-HT1A partial agonism approved by the U.S. Food and Drug Administration for the treatment of MDD, besides schizophrenia in adults. The clinical trials leading to the extended approval of brexpiprazole rely on the definition of 'inadequate response' to antidepressants, which seems to poorly represent the most severe cases of TRD seen in clinical practice. TRD definitions appraised in the literature are likewise inconsistent and questionable from a clinical-standpoint. Compared to aripiprazole, brexpiprazole has lower D-2 intrinsic activity, although the latter features a more potent serotonergic 5-HT2A antagonism. The actual propensity of brexpiprazole to induce akathisia and tardive dyskinesia warrants assessment by ad-hoc designed long-term, controlled trials.
机译:介绍:抗治疗抑郁症(TRD),很少可互换称为“抑郁症不充分应对标准抗抑郁药物”,带来了重大负担。非典型抗精神病药代表了一种抗抑郁抑郁症的流行增强策略,尽管它们的功效/安全性曲线在不同的药剂上变化和抑郁症的演示文稿。涵盖了地区:本综述评估支持使用Breskiprazole增强用于主要抑郁症(MDD)成人使用的证据表明对标准抗抑郁药的反应不足,涵盖相关的监管事务和基本药理学。专家意见:Brengiprazole是一种“第三代”抗精神病药,其具有由美国食品和药物管理局批准的多巴胺能D-2和Serotonergic 5-HT1A部分激动症,用于治疗MDD,除了成年人的精神分裂症。临床试验导致Breskiprazole延长批准依赖于对抗抑郁药的“不足反应”的定义,这似乎似乎代表临床实践中最严重的TRD病例。在文献中评估的TRD定义同样不一致,可从临床角度出发。与阿里普哌唑相比,Breskiprazole具有较低的D-2内在活性,尽管后者具有更有效的血清ond 5-HT2A拮抗作用。 Brengiprazole诱导Akathisia和Tardive Dyskinesia的实际倾向通过Ad-Hoc设计的长期受控试验进行评估。

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