From the Centre for Psychedelic Research, Department of Brain Sciences, Faculty of Medicine, Imperial College London, London.
N Engl J Med. 2021 Apr 15;384(15):1402-1411. doi: 10.1056/NEJMoa2032994.
Psilocybin may have antidepressant properties, but direct comparisons between psilocybin and established treatments for depression are lacking.
In a phase 2, double-blind, randomized, controlled trial involving patients with long-standing, moderate-to-severe major depressive disorder, we compared psilocybin with escitalopram, a selective serotonin-reuptake inhibitor, over a 6-week period. Patients were assigned in a 1:1 ratio to receive two separate doses of 25 mg of psilocybin 3 weeks apart plus 6 weeks of daily placebo (psilocybin group) or two separate doses of 1 mg of psilocybin 3 weeks apart plus 6 weeks of daily oral escitalopram (escitalopram group); all the patients received psychological support. The primary outcome was the change from baseline in the score on the 16-item Quick Inventory of Depressive Symptomatology-Self-Report (QIDS-SR-16; scores range from 0 to 27, with higher scores indicating greater depression) at week 6. There were 16 secondary outcomes, including QIDS-SR-16 response (defined as a reduction in score of >50%) and QIDS-SR-16 remission (defined as a score of ≤5) at week 6.
A total of 59 patients were enrolled; 30 were assigned to the psilocybin group and 29 to the escitalopram group. The mean scores on the QIDS-SR-16 at baseline were 14.5 in the psilocybin group and 16.4 in the escitalopram group. The mean (±SE) changes in the scores from baseline to week 6 were -8.0±1.0 points in the psilocybin group and -6.0±1.0 in the escitalopram group, for a between-group difference of 2.0 points (95% confidence interval [CI], -5.0 to 0.9) (P = 0.17). A QIDS-SR-16 response occurred in 70% of the patients in the psilocybin group and in 48% of those in the escitalopram group, for a between-group difference of 22 percentage points (95% CI, -3 to 48); QIDS-SR-16 remission occurred in 57% and 28%, respectively, for a between-group difference of 28 percentage points (95% CI, 2 to 54). Other secondary outcomes generally favored psilocybin over escitalopram, but the analyses were not corrected for multiple comparisons. The incidence of adverse events was similar in the trial groups.
On the basis of the change in depression scores on the QIDS-SR-16 at week 6, this trial did not show a significant difference in antidepressant effects between psilocybin and escitalopram in a selected group of patients. Secondary outcomes generally favored psilocybin over escitalopram, but the analyses of these outcomes lacked correction for multiple comparisons. Larger and longer trials are required to compare psilocybin with established antidepressants. (Funded by the Alexander Mosley Charitable Trust and Imperial College London's Centre for Psychedelic Research; ClinicalTrials.gov number, NCT03429075.).
裸盖菇素可能具有抗抑郁作用,但缺乏裸盖菇素与现有抗抑郁治疗方法的直接比较。
在一项涉及患有长期、中度至重度重度抑郁症患者的 2 期、双盲、随机、对照试验中,我们比较了 6 周内使用裸盖菇素与选择性 5-羟色胺再摄取抑制剂(SSRI)依地普仑的情况。患者以 1:1 的比例随机分配接受两次 25 毫克裸盖菇素,间隔 3 周,加 6 周每日安慰剂(裸盖菇素组)或两次 1 毫克裸盖菇素,间隔 3 周,加 6 周每日口服依地普仑(依地普仑组);所有患者均接受心理支持。主要结局是第 6 周时自我报告的 16 项快速抑郁症状清单(QIDS-SR-16)评分从基线的变化;评分范围为 0 至 27,分数越高表示抑郁程度越严重)。有 16 个次要结局,包括 QIDS-SR-16 反应(定义为评分下降>50%)和 QIDS-SR-16 缓解(定义为评分≤5)在第 6 周。
共有 59 名患者入组;30 名被分配到裸盖菇素组,29 名被分配到依地普仑组。裸盖菇素组基线时 QIDS-SR-16 的平均得分为 14.5,依地普仑组为 16.4。从基线到第 6 周,裸盖菇素组的评分变化平均值为-8.0±1.0 分,依地普仑组为-6.0±1.0 分,两组间差异为 2.0 分(95%置信区间[CI],-5.0 至 0.9)(P=0.17)。裸盖菇素组 70%的患者出现 QIDS-SR-16 反应,依地普仑组为 48%,两组间差异为 22 个百分点(95%CI,-3 至 48);QIDS-SR-16 缓解分别为 57%和 28%,两组间差异为 28 个百分点(95%CI,2 至 54)。其他次要结局通常有利于裸盖菇素而不是依地普仑,但分析未对多次比较进行校正。试验组的不良事件发生率相似。
根据第 6 周 QIDS-SR-16 抑郁评分的变化,本试验未显示在选定患者群体中裸盖菇素与依地普仑在抗抑郁作用方面有显著差异。次要结局通常有利于裸盖菇素而不是依地普仑,但这些结局的分析缺乏对多次比较的校正。需要更大和更长的试验来比较裸盖菇素与现有的抗抑郁药。(由亚历山大莫斯利慈善信托基金和帝国理工学院的迷幻研究中心资助;临床试验.gov 编号,NCT03429075。)
