DigiHealth Institute, Neu-Ulm University of Applied Sciences, Neu-Ulm, Germany.
Institute for Health Services Research and Health Economics, Centre for Health and Society, Medical Faculty and University Hospital Düsseldorf, Heinrich-Heine University, Düsseldorf, Germany.
Cochrane Database Syst Rev. 2021 Dec 17;12(12):CD013304. doi: 10.1002/14651858.CD013304.pub2.
Typical and atypical antipsychotics are widely used to treat agitation and psychosis in dementia. However, whether or not they are beneficial is uncertain. Some trials have yielded negative results and effectiveness may be outweighed by harms.
To assess the efficacy and safety of antipsychotics for the treatment of agitation and psychosis in people with Alzheimer's disease and vascular dementia.
We searched ALOIS, the Cochrane Dementia and Cognitive Improvement Group's register, MEDLINE (Ovid Sp), Embase (Ovid SP), PsycINFO (Ovid SP), CINAHL (EBSCOhost), Web of Science Core Collection (ISI Web of Science), LILACS (BIREME), ClinicalTrials.gov and the World Health Organization's meta-register, and the International Clinical Trials Registry Portal on 7 January 2021. Two review authors independently screened the title and abstract of the hits, and two review authors assessed the full text of studies that got through this screening.
We included randomised, placebo-controlled, parallel-arm trials comparing the effects of antipsychotics and placebo for the treatment of agitation or psychosis in people with dementia due to Alzheimer's disease or vascular dementia, or both, irrespective of age, severity of cognitive impairment, and setting. (The majority of) participants had to have clinically significant agitation (including aggression) or psychosis or both at baseline. We excluded studies about antipsychotics that are no longer available in the USA or EU, or that are used for emergency short-term sedation. We also excluded head-to-head trials and antipsychotic withdrawal trials.
The primary outcomes were (1) reduction in agitation or psychosis in participants with agitation or psychosis, respectively at baseline, and (2) the number of participants with adverse events: somnolence, extrapyramidal symptoms, any adverse event, any serious adverse event (SAE), and death. Two review authors independently extracted the necessary data and assessed risk of bias with the Cochrane risk of bias tool. We calculated the pooled effect on agitation and psychosis for typical and atypical antipsychotics separately, and the pooled risk of adverse effects independent of the target symptom (agitation or psychosis). We used RevMan Web for the analyses.
The search yielded 8233 separate hits. After assessing the full-text of 35 studies, we included 24 trials that met the eligibility criteria. Six trials tested a typical antipsychotic, four for agitation and two for psychosis. Twenty trials tested an atypical antipsychotic, eight for agitation and 12 for psychosis. Two trials tested both drug types. Seventeen of 26 comparisons were performed in patients with Alzheimer's disease specifically. The other nine comparisons also included patients with vascular dementia or mixed dementia. Together, the studies included 6090 participants (12 to 652 per study). The trials were performed in institutionalised, hospitalised and community-dwelling patients, or a combination of those. For typical antipsychotics (e.g. haloperidol, thiothixene), we are uncertain whether these drugs improve agitation compared with placebo (standardised mean difference (SMD) -0.36, 95% confidence interval (CI) -0.57 to -0.15, 4 studies, n = 361); very low-certainty evidence, but typical antipsychotics may improve psychosis slightly (SMD -0.29, 95% CI -0.55 to -0.03, 2studies, n= 240; low-certainty evidence) compared with placebo. These drugs probably increase the risk of somnolence (risk ratio (RR) 2.62, 95% CI 1.51 to 4.56, 3 studies, n = 466; moderate-certainty evidence) and increase extrapyramidal symptoms (RR 2.26, 95% CI 1.58 to 3.23, 3 studies, n = 467; high-certainty) evidence. There was no evidence regarding the risk of any adverse event. The risks of SAEs (RR 1.32, 95% CI 0.65 to 2.66, 1 study, n = 193) and death (RR 1.46, 95% CI 0.54 to 4.00, 6 studies, n = 578) may be increased slightly, but these estimates were very imprecise, and the certainty was low. The effect estimates for haloperidol from five trials were in line with those of the drug class. Atypical antipsychotics (e.g. risperidone, olanzapine, aripiprazole, quetiapine) probably reduce agitation slightly (SMD -0.21, 95% CI -0.30 to -0.12, 7 studies, n = 1971; moderate-certainty evidence), but probably have a negligible effect on psychosis (SMD -0.11, 95% CI -0.18 to -0.03, 12 studies, n = 3364; moderate-certainty evidence). These drugs increase the risk of somnolence (RR 1.93, 95% CI 1.57 to 2.39, 13 studies, n - 3878; high-certainty evidence) and are probably also associated with slightly increased risk of extrapyramidal symptoms (RR 1.39, 95% CI 1.14 to 1.68, 15 studies, n = 4180; moderate-certainty evidence), serious adverse events (RR 1.32, 95% CI 1.09 to 1.61, 15 studies, n= 4316; moderate-certainty evidence) and death (RR 1.36, 95% CI 0.90 to 2.05, 17 studies, n= 5032; moderate-certainty evidence), although the latter estimate was imprecise. The drugs probably have a negligible effect on the risk of any adverse event (RR 1.05, 95% CI 1.02 to 1.09, 11 studies, n = 2785; moderate-certainty evidence). The findings from seven trials for risperidone were in line with those for the drug class.
AUTHORS' CONCLUSIONS: There is some evidence that typical antipsychotics might decrease agitation and psychosis slightly in patients with dementia. Atypical antipsychotics reduce agitation in dementia slightly, but their effect on psychosis in dementia is negligible. The apparent effectiveness of the drugs seen in daily practice may be explained by a favourable natural course of the symptoms, as observed in the placebo groups. Both drug classes increase the risk of somnolence and other adverse events. If antipsychotics are considered for sedation in patients with severe and dangerous symptoms, this should be discussed openly with the patient and legal representative.
典型和非典型抗精神病药被广泛用于治疗痴呆患者的激越和精神病。然而,其是否有效尚不确定。一些试验得出了阴性结果,而且其益处可能被危害所抵消。
评估抗精神病药治疗阿尔茨海默病和血管性痴呆患者激越和精神病的疗效和安全性。
我们检索了 ALOIS、Cochrane 痴呆和认知改善组的注册库、MEDLINE(Ovid Sp)、Embase(Ovid SP)、PsycINFO(Ovid SP)、CINAHL(EBSCOhost)、Web of Science 核心合集(ISI Web of Science)、LILACS(BIREME)、ClinicalTrials.gov 和世界卫生组织的荟萃分析注册库,并于 2021 年 1 月 7 日检索了国际临床试验注册平台。两名综述作者独立筛选标题和摘要,两名综述作者评估通过筛选的研究的全文。
我们纳入了随机、安慰剂对照、平行臂试验,比较了抗精神病药和安慰剂治疗痴呆患者激越或精神病的效果,这些患者的痴呆病因是阿尔茨海默病或血管性痴呆,或两者兼有,无论年龄、认知障碍严重程度和环境如何。(大多数)参与者在基线时均有明显的激越(包括攻击)或精神病或两者兼有。我们排除了那些在美国或欧盟不再可用的、或用于紧急短期镇静的抗精神病药的研究。我们还排除了头对头试验和抗精神病药撤药试验。
主要结局是(1)基线时有激越或精神病的参与者激越或精神病的减少,和(2)出现不良事件的参与者人数:嗜睡、锥体外系症状、任何不良事件、任何严重不良事件(SAE)和死亡。两名综述作者独立提取必要的数据,并使用 Cochrane 偏倚风险工具评估风险偏倚。我们分别对典型和非典型抗精神病药的激越和精神病进行了荟萃分析,并对目标症状(激越或精神病)以外的不良反应风险进行了荟萃分析。我们使用 RevMan Web 进行分析。
搜索产生了 8233 个单独的结果。在评估了 35 项研究的全文后,我们纳入了符合纳入标准的 24 项试验。6 项试验测试了一种典型的抗精神病药,其中 4 项用于激越,2 项用于精神病。20 项试验测试了一种非典型的抗精神病药,其中 8 项用于激越,12 项用于精神病。两项试验同时测试了两种药物类型。26 项比较中有 17 项是在专门针对阿尔茨海默病患者进行的。其他 9 项比较也包括血管性痴呆或混合性痴呆患者。这些研究共纳入了 6090 名参与者(每个研究 12 至 652 人)。这些试验在住院患者、社区居民或这些人群的组合中进行。对于典型的抗精神病药(如氟哌啶醇、硫利达嗪),我们不确定这些药物是否能改善激越与安慰剂相比(标准化均数差(SMD)-0.36,95%置信区间(CI)-0.57 至-0.15,4 项研究,n = 361;低质量证据);但典型抗精神病药可能会略微改善精神病(SMD-0.29,95%CI-0.55 至-0.03,2 项研究,n=240;低质量证据)。与安慰剂相比。这些药物可能会增加嗜睡的风险(风险比(RR)2.62,95%CI 1.51 至 4.56,3 项研究,n = 466;中等质量证据)和增加锥体外系症状(RR 2.26,95%CI 1.58 至 3.23,3 项研究,n = 467;高质量证据)的风险。没有关于任何不良事件风险的证据。SAE(RR 1.32,95%CI 0.65 至 2.66,1 项研究,n = 193)和死亡(RR 1.46,95%CI 0.54 至 4.00,6 项研究,n = 578)的风险可能略有增加,但这些估计值非常不精确,质量较低。五项试验中氟哌啶醇的效应估计值与药物类别一致。非典型抗精神病药(如利培酮、奥氮平、阿立哌唑、喹硫平)可能会略微减少激越(SMD-0.21,95%CI-0.30 至-0.12,7 项研究,n = 1971;中等质量证据),但对精神病的影响可能可以忽略不计(SMD-0.11,95%CI-0.18 至-0.03,12 项研究,n = 3364;中等质量证据)。这些药物增加嗜睡的风险(RR 1.93,95%CI 1.57 至 2.39,13 项研究,n = 3878;高质量证据),并且可能与锥体外系症状的风险增加也有一定关系(RR 1.39,95%CI 1.14 至 1.68,15 项研究,n = 4180;中等质量证据)、严重不良事件(RR 1.32,95%CI 1.09 至 1.61,15 项研究,n = 4316;中等质量证据)和死亡(RR 1.36,95%CI 0.90 至 2.05,17 项研究,n = 5032;中等质量证据),尽管后者的估计值不太精确。这些药物可能对任何不良事件的风险没有影响(RR 1.05,95%CI 1.02 至 1.09,11 项研究,n = 2785;中等质量证据)。利培酮的七项试验结果与药物类别一致。
有一些证据表明,典型抗精神病药可能会稍微减轻痴呆患者的激越和精神病。非典型抗精神病药可轻微减轻痴呆患者的激越,但对痴呆患者的精神病影响可忽略不计。在日常实践中观察到的药物疗效可能是由于症状的自然病程有利,这可能是由于症状的自然病程有利。两种药物类别均增加嗜睡和其他不良反应的风险。如果考虑抗精神病药用于治疗严重和危险症状的镇静,应与患者和法定代表公开讨论。
