Department of Old Age Psychiatry, King's College London, London, UK.
Medical Research Council Population Health Research Unit, University of Oxford, Oxford, UK.
Health Technol Assess. 2018 Nov;22(67):1-62. doi: 10.3310/hta22670.
Very late-onset (aged ≥ 60 years) schizophrenia-like psychosis (VLOSLP) occurs frequently but no placebo-controlled, randomised trials have assessed the efficacy or risks of antipsychotic treatment. Most patients are not prescribed treatment.
The study investigated whether or not low-dose amisulpride is superior to placebo in reducing psychosis symptoms over 12 weeks and if any benefit is maintained by continuing treatment thereafter. Treatment safety and cost-effectiveness were also investigated.
Three-arm, parallel-group, placebo-controlled, double-blind, randomised controlled trial. Participants who received at least one dose of study treatment were included in the intention-to-treat analyses.
Secondary care specialist old age psychiatry services in 25 NHS mental health trusts in England and Scotland.
Patients meeting diagnostic criteria for VLOSLP and scoring > 30 points on the Brief Psychiatric Rating Scale (BPRS).
Participants were randomly assigned to three arms in a two-stage trial: (1) 100 mg of amisulpride in both stages, (2) amisulpride then placebo and (3) placebo then amisulpride. Treatment duration was 12 weeks in stage 1 and 24 weeks (later reduced to 12) in stage 2. Participants, investigators and outcome assessors were blind to treatment allocation.
Primary outcomes were psychosis symptoms assessed by the BPRS and trial treatment discontinuation for non-efficacy. Secondary outcomes were extrapyramidal symptoms measured with the Simpson-Angus Scale, quality of life measured with the World Health Organization's quality-of-life scale, and cost-effectiveness measured with NHS, social care and carer work loss costs and EuroQol-5 Dimensions.
A total of 101 participants were randomised. Ninety-two (91%) participants took the trial medication, 59 (64%) completed stage 1 and 33 (56%) completed stage 2 treatment. Despite suboptimal compliance, improvements in BPRS scores at 12 weeks were 7.7 points (95% CI 3.8 to 11.5 points) greater with amisulpride than with placebo (11.9 vs. 4.2 points; = 0.0002). In stage 2, BPRS scores improved by 1.1 point in those who continued with amisulpride but deteriorated by 5.2 points in those who switched from amisulpride to placebo, a difference of 6.3 points (95% CI 0.9 to 11.7 points; = 0.024). Fewer participants allocated to the amisulpride group stopped treatment because of non-efficacy in stages 1 ( = 0.01) and 2 ( = 0.031). The number of patients stopping because of extrapyramidal symptoms and other side effects did not differ significantly between groups. Amisulpride treatment in the base-case analyses was associated with non-significant reductions in combined NHS, social care and unpaid carer costs and non-significant reductions in quality-adjusted life-years (QALYs) in both stages. Including patients who were intensive users of inpatient services in sensitivity analyses did not change the QALY result but resulted in placebo dominance in stage 1 and significant reductions in NHS/social care (95% CI -£8923 to -£122) and societal costs (95% CI -£8985 to -£153) for those continuing with amisulpride.
The original recruitment target of 300 participants was not achieved and compliance with trial medication was highly variable.
Low-dose amisulpride is effective and well tolerated as a treatment for VLOSLP, with benefits maintained by prolonging treatment. Potential adverse events include clinically significant extrapyramidal symptoms and falls.
Trials should examine the longer-term effectiveness and safety of antipsychotic treatment in this patient group, and assess interventions to improve their appreciation of potential benefits of antipsychotic treatment and compliance with prescribed medication.
Current Controlled Trials ISRCTN45593573 and EudraCT2010-022184-35.
This project was funded by the National Institute for Health Research (NIHR) Health Technology Assessment programme and will be published in full in ; Vol. 22, No. 67. See the NIHR Journals Library website for further project information.
极晚发性(年龄≥60 岁)精神分裂症样精神病(VLOSLP)经常发生,但尚无安慰剂对照、随机试验评估抗精神病药物治疗的疗效或风险。大多数患者未接受治疗。
本研究旨在评估低剂量氨磺必利是否优于安慰剂,能否在 12 周内减轻精神病症状,以及在此后的治疗中是否能保持任何益处。还研究了治疗安全性和成本效益。
三臂、平行组、安慰剂对照、双盲、随机对照试验。至少接受一次研究治疗的参与者被纳入意向治疗分析。
英格兰和苏格兰 25 个 NHS 心理健康信托机构的二级保健专科老年精神病服务。
符合 VLOSLP 诊断标准且简明精神病评定量表(BPRS)评分>30 分的患者。
参与者在两阶段试验中随机分配至三组:(1)氨磺必利 100mg 用于两个阶段,(2)氨磺必利后安慰剂,(3)安慰剂后氨磺必利。第一阶段的治疗持续时间为 12 周,第二阶段为 24 周(后来减少至 12 周)。参与者、研究者和结局评估者对治疗分配不知情。
主要结局是用 BPRS 评估精神病症状和因无效而停止治疗。次要结局是用 Simpson-Angus 量表测量的锥体外系症状、用世界卫生组织生活质量量表测量的生活质量,以及用 NHS、社会护理和护理人员工作损失成本和 EuroQol-5 维度测量的成本效益。
共有 101 名参与者被随机分配。92 名(91%)参与者服用了试验药物,59 名(64%)完成了第一阶段治疗,33 名(56%)完成了第二阶段治疗。尽管依从性不理想,但与安慰剂相比,氨磺必利在 12 周时 BPRS 评分的改善高 7.7 分(95%CI 3.8 至 11.5 分;=0.0002)。在第二阶段,继续使用氨磺必利的患者 BPRS 评分改善 1.1 分,而从氨磺必利转换为安慰剂的患者恶化 5.2 分,差异为 6.3 分(95%CI 0.9 至 11.7 分;=0.024)。在第一阶段(=0.01)和第二阶段(=0.031),因无效而停止治疗的接受氨磺必利治疗的参与者人数较少。各组因锥体外系症状和其他副作用而停止治疗的人数没有显著差异。在两阶段的基础病例分析中,氨磺必利治疗与 NHS、社会护理和非付费护理人员成本的联合减少无关,且与质量调整生命年(QALYs)的非显著减少有关。在敏感性分析中纳入了住院服务密集使用者的患者并未改变 QALY 结果,但在第一阶段导致安慰剂优势,且显著降低 NHS/社会护理(95%CI -£8923 至 -£122)和社会成本(95%CI -£8985 至 -£153)对于继续使用氨磺必利的患者。
最初招募 300 名参与者的目标没有实现,试验药物的依从性高度可变。
低剂量氨磺必利治疗极晚发性精神分裂症样精神病有效且耐受良好,延长治疗可保持疗效。潜在的不良事件包括临床意义上的锥体外系症状和跌倒。
试验应检查该患者群体中抗精神病药物治疗的长期有效性和安全性,并评估干预措施,以提高他们对潜在益处的认识和对处方药物的依从性。
当前对照试验 ISRCTN45593573 和 EudraCT2010-022184-35。
本项目由英国国家卫生研究院(NIHR)健康技术评估计划资助,将全文在 ; 第 22 卷,第 67 期。欲了解更多项目信息,请访问 NIHR 期刊库网站。
