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慢工出细活?抗精神病药停药率、剂量与精神病复发风险。

Does Slow and Steady Win the Race? Rates of Antipsychotic Discontinuation, Antipsychotic Dose, and Risk of Psychotic Relapse.

机构信息

Department of Psychiatry, University of Oxford, Oxford, UK.

Oxford Health NHS Foundation Trust, Oxford, UK.

出版信息

Schizophr Bull. 2024 Apr 30;50(3):513-520. doi: 10.1093/schbul/sbad139.

Abstract

BACKGROUND

Antipsychotics are recommended for prevention of relapse in schizophrenia. It is unclear whether increased risk of relapse following antipsychotic discontinuation is predominantly associated with an absolute magnitude of dose reduction or rate of antipsychotic reduction. Establishing the responsible mechanism is important because prolonged withdrawal schedules have been suggested to reduce risk of relapse.

STUDY DESIGN

Individual patient data from antipsychotic discontinuation studies were obtained. We estimated the occupancy of receptors over time using half-lives and median effective dose ED50 values obtained from pharmacokinetic and receptor occupancy studies. Hazard ratios for relapse events were calculated using Cox proportional hazards models to assess the influence of formulation (oral, 1-monthly, and 3-monthly injections). The change in hazard ratio over time was estimated, and the effect of time-varying covariates was calculated, including rate of occupancy reduction and absolute receptor occupancy.

STUDY RESULTS

Five studies including 1388 participants with schizophrenia were identified (k = 2: oral, k = 2: 1-monthly injection, k = 1: 3-monthly injection). Withdrawal of long-acting injectable medication did not lead to a lower hazard ratio compared with withdrawal of oral medication, and this included the period immediately following randomization. Hazard ratios were not associated with the rate of decline of receptor occupancy; however, they were associated with reduced absolute occupancy in trials of long-acting injections (P = .038).

CONCLUSIONS

Antipsychotic discontinuation is associated with an increased risk of psychotic relapse, related to receptor occupancy. Although relapse does not appear to be related to the rate of discontinuation, gradual discontinuation strategies may allow for easier antipsychotic reinstatement in case of symptomatic worsening.

摘要

背景

抗精神病药被推荐用于预防精神分裂症复发。目前尚不清楚抗精神病药停药后复发风险增加是主要与剂量减少的绝对幅度还是抗精神病药减少的速度有关。确定负责的机制很重要,因为已经提出延长停药方案可以降低复发风险。

研究设计

从抗精神病药停药研究中获得了个体患者数据。我们使用半衰期和从中获得的药效学和受体占有率研究获得的中效剂量 ED50 值来估算受体随时间的占有率。使用 Cox 比例风险模型计算复发事件的风险比,以评估制剂(口服、每月 1 次和每 3 个月 1 次注射)的影响。估计风险比随时间的变化,并计算时间变化的协变量的影响,包括占有率减少的速度和绝对受体占有率。

研究结果

确定了五项包括 1388 名精神分裂症患者的研究(k=2:口服,k=2:每月 1 次注射,k=1:每 3 个月 1 次注射)。与口服药物停药相比,长效注射药物停药并不会导致较低的风险比,包括随机分组后立即停药的时期。风险比与受体占有率下降的速度无关;然而,它们与长效注射试验中的绝对占有率降低有关(P=0.038)。

结论

抗精神病药停药与精神病复发风险增加有关,与受体占有率有关。尽管复发似乎与停药速度无关,但在症状恶化时,逐渐停药策略可能更容易重新开始使用抗精神病药。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/042e/11059789/e689de106f1c/sbad139_fig1.jpg

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