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氯胺酮治疗重度抑郁症:一项系统评价与荟萃分析。

Ketamine for the treatment of major depression: a systematic review and meta-analysis.

作者信息

Nikolin Stevan, Rodgers Anthony, Schwaab Andreas, Bahji Anees, Zarate Carlos, Vazquez Gustavo, Loo Colleen

机构信息

Discipline of Psychiatry and Mental Health, University of New South Wales, Sydney, Australia.

Black Dog Institute, Sydney, Australia.

出版信息

EClinicalMedicine. 2023 Aug 3;62:102127. doi: 10.1016/j.eclinm.2023.102127. eCollection 2023 Aug.

Abstract

BACKGROUND

Intranasal esketamine has received regulatory approvals for the treatment of depression. Recently a large trial of repeated dose racemic ketamine also demonstrated efficacy in severe depression. However, uncertainties remain regarding comparative efficacy, dosage, and the time course of response.

METHODS

In this systematic review and meta-analysis, we searched Embase, Medline, Pubmed, PsycINFO, and CENTRAL up to April 13, 2023, for randomised controlled trials (RCTs) investigating ketamine for depression. Two investigators independently assessed study eligibility and risk of bias and extracted the data on depression severity scores, response and remission rates, and all-cause dropouts. Multivariable mixed-effects meta-regressions incorporated drug formulation (racemic (Rac) or esketamine (Esket)) and dose (Low or High) as covariates. Treatment effects were assessed: immediately following the first dose, during further repeated dosing, and follow-up after the final dose of a treatment course. This study is registered with PROSPERO (CRD42021221157).

FINDINGS

The systematic review identified 687 articles, of which 49 RCTs were eligible for analysis, comprising 3299 participants. Standardised mean differences (95% confidence intervals) immediately following the first/single treatment were moderate-high for all conditions (Rac-High: -0.73, -0.91 to -0.56; Esket-High: -0.48, -0.75 to -0.20; Rac-Low: -0.33, -0.54 to -0.12; Esket-Low: -0.55, -0.87 to -0.24). Ongoing effects during repeated dosing were significantly greater than the control for Rac-High (-0.61; -1.02 to -0.20) and Rac-Low (-0.55, -1.09 to -0.00), but not Esket-Low (-0.15, -0.49 to 0.19) or Esket-High (-0.22, -0.54 to 0.10). At follow-up effects remained significant for racemic ketamine (-0.65; -1.23 to -0.07) but not esketamine (-0.33; -0.96 to 0.31). All-cause dropout was similar between experiment and control conditions for both formulations combined (Odds Ratio = 1.18, 0.85-1.64). Overall heterogeneity varied from 5.7% to 87.6.

INTERPRETATION

Our findings suggested that effect sizes for depression severity, as well as response and remission rates, were numerically greater for racemic ketamine than esketamine. Higher doses were more effective than low doses. Differences were evident in initial effects, ongoing treatment, and lasting effects after the final dose.

FUNDING

None.

摘要

背景

鼻内用艾司氯胺酮已获得治疗抑郁症的监管批准。最近一项关于重复剂量消旋氯胺酮的大型试验也证明了其对重度抑郁症的疗效。然而,在比较疗效、剂量和反应的时间过程方面仍存在不确定性。

方法

在这项系统评价和荟萃分析中,我们检索了截至2023年4月13日的Embase、Medline、Pubmed、PsycINFO和CENTRAL数据库,以查找研究氯胺酮治疗抑郁症的随机对照试验(RCT)。两名研究人员独立评估研究的纳入资格和偏倚风险,并提取抑郁症严重程度评分、缓解率和全因脱落率的数据。多变量混合效应荟萃回归将药物制剂(消旋体(Rac)或艾司氯胺酮(Esket))和剂量(低或高)作为协变量。评估治疗效果:在首次给药后立即、进一步重复给药期间以及一个疗程的最后一剂后的随访期间。本研究已在PROSPERO(CRD42021221157)注册。

结果

系统评价共识别出687篇文章,其中49项RCT符合分析条件,共3299名参与者。在所有情况下,首次/单次治疗后立即出现的标准化平均差(95%置信区间)为中度至高度(Rac-高剂量组:-0.73,-0.91至-0.56;Esket-高剂量组:-0.48,-0.75至-0.20;Rac-低剂量组:-0.33,-0.54至-0.12;Esket-低剂量组:-0.55,-0.87至-0.24)。重复给药期间的持续效应显著大于对照组,Rac-高剂量组(-0.61;-1.02至-0.20)和Rac-低剂量组(-0.55,-1.09至-0.00),但Esket-低剂量组(-0.15,-0.49至0.19)和Esket-高剂量组(-0.22,-0.54至0.10)则不然。在随访时,消旋氯胺酮的效应仍然显著(-0.65;-1.23至-0.07),但艾司氯胺酮则不然(-0.33;-0.96至0.31)。两种制剂合并后,实验和对照条件下的全因脱落率相似(优势比=1.18,0.85-1.64)。总体异质性从5.7%到87.6%不等。

解读

我们的研究结果表明,消旋氯胺酮在抑郁症严重程度、缓解率和反应率方面的效应量在数值上大于艾司氯胺酮。高剂量比低剂量更有效。在初始效应、持续治疗和最后一剂后的持久效应方面存在明显差异。

资金来源

无。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a033/10430179/36c29b398432/gr1.jpg

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