Correll Christoph U, Leucht Stefan, Kane John M
Department of Psychiatry Research, Zucker Hillside Hospital, North Shore-Long Island Jewish Health System, Schneider Children's Hospital, Glen Oaks, NY 11004, USA.
Am J Psychiatry. 2004 Mar;161(3):414-25. doi: 10.1176/appi.ajp.161.3.414.
Based on lower rates of acute extrapyramidal side effects associated with second-generation antipsychotics, compared to first-generation antipsychotics, and based on preliminary data, second-generation antipsychotics are expected to cause less tardive dyskinesia than first-generation antipsychotics. This hypothesis was examined in a systematic review of studies involving open or controlled treatment with any second-generation antipsychotic.
Studies of treatment with second-generation antipsychotics lasting > or =1 year and reporting on new cases of tardive dyskinesia or dyskinesia were systematically reviewed.
In 11 studies, 2,769 patients received treatment with risperidone (five studies, N=1,235), olanzapine (two studies, N=610), quetiapine (two studies, N=386), amisulpride (one study, N=331), or ziprasidone (one study, N=207) for a weighted mean and median duration of 263 and 306 days, respectively. Study designs were double blind and randomized (N=3); open-label extensions of double-blind, randomized trials (N=4); and open label (N=4). Of the four trials that had a comparator (all involving adults with schizophrenia spectrum disorders), three used haloperidol (N=408) and one used placebo (N=71). Studied populations included children (N=77), adults (N=1,419), adults and elderly persons (N=794), and exclusively patients age 54 years or older (N=479). The weighted mean annual incidence of tardive dyskinesia for second-generation antipsychotics was 0% in the children, 0.8% (range=0.0%-1.5%) in the adults, 6.8% in the mixed adult and elderly population, and 5.3% (range=0.0%-13.4%) in the patients age 54 years and older, compared to 5.4% (range=4.1%-7.4%) in adults treated with haloperidol.
Results from 11 long-term studies support the idea that second-generation antipsychotics have a reduced risk for tardive dyskinesia, compared to first-generation antipsychotics, although the doses of haloperidol used in the comparator studies were relatively high. More carefully designed studies, ideally lasting beyond 1 year and comparing the effects of different second-generation antipsychotics in patients who have never taken first-generation antipsychotics, are needed to estimate the true risk. It would not appear premature for clinicians to consider these findings in making long-term treatment decisions.
与第一代抗精神病药物相比,第二代抗精神病药物的急性锥体外系副作用发生率较低,且基于初步数据,预计第二代抗精神病药物导致迟发性运动障碍的可能性低于第一代抗精神病药物。本研究通过系统回顾涉及任何第二代抗精神病药物开放或对照治疗的研究来检验这一假设。
系统回顾了使用第二代抗精神病药物治疗持续≥1年且报告迟发性运动障碍或运动障碍新病例的研究。
在11项研究中,2769例患者接受了利培酮(5项研究,N = 1235)、奥氮平(2项研究,N = 610)、喹硫平(2项研究,N = 386)、氨磺必利(1项研究,N = 331)或齐拉西酮(1项研究,N = 207)治疗,加权平均和中位治疗持续时间分别为263天和306天。研究设计包括双盲随机试验(N = 3);双盲随机试验的开放标签扩展试验(N = 4);以及开放标签试验(N = 4)。在四项有对照的试验中(均涉及精神分裂症谱系障碍成人患者),三项使用氟哌啶醇(N = 408),一项使用安慰剂(N = 71)。研究人群包括儿童(N = 77)、成人(N = 1419)、成人和老年人(N = 794)以及年龄54岁及以上的患者(N = 479)。第二代抗精神病药物迟发性运动障碍的加权平均年发生率在儿童中为0%,成人中为0.8%(范围 = 0.0% - 1.5%),成人和老年人混合人群中为6.8%,54岁及以上患者中为5.3%(范围 = 0.0% - 13.4%),而使用氟哌啶醇治疗的成人中为5.4%(范围 = 4.1% - 7.4%)。
11项长期研究的结果支持以下观点:与第一代抗精神病药物相比,第二代抗精神病药物导致迟发性运动障碍的风险降低,尽管对照研究中使用的氟哌啶醇剂量相对较高。需要更精心设计的研究,理想情况下持续时间超过1年,并比较不同第二代抗精神病药物对从未服用过第一代抗精神病药物患者的影响,以估计真正的风险。临床医生在做出长期治疗决策时考虑这些发现似乎并不为时过早。
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