在双相躁狂症患者的对照研究中,喹硫平所致锥体外系症状(EPS)的安慰剂水平发生率。
Placebo-level incidence of extrapyramidal symptoms (EPS) with quetiapine in controlled studies of patients with bipolar mania.
作者信息
Nasrallah Henry A, Brecher Martin, Paulsson Björn
机构信息
University of Cincinnati College of Medicine, Cincinnati, OH, USA.
出版信息
Bipolar Disord. 2006 Oct;8(5 Pt 1):467-74. doi: 10.1111/j.1399-5618.2006.00350.x.
OBJECTIVES
To evaluate extrapyramidal symptoms (EPS), including akathisia, with quetiapine in patients with bipolar mania.
METHODS
Data were analyzed from four similarly designed, randomized, double-blind, 3- to 12-week studies. Two studies evaluated quetiapine monotherapy (up to 800 mg/day) (n = 209) versus placebo (n = 198), with lithium or haloperidol monotherapy as respective active controls. Two studies evaluated quetiapine (up to 800 mg/day) in combination with a mood stabilizer (lithium or divalproex, QTP + Li/DVP) (n = 196) compared to placebo and mood stabilizer (PBO + Li/DVP) (n = 203). Extrapyramidal symptoms were evaluated using the Simpson-Angus Scale (SAS), the Barnes Akathisia Rating Scale (BARS), adverse event reports and anticholinergic drug usage.
RESULTS
The incidence of EPS-related adverse events, including akathisia, was no different with quetiapine monotherapy (12.9%) than with placebo (13.1%). Similarly, EPS-related adverse events with QTP + Li/DVP (21.4%) were no different than with PBO + Li/DVP (19.2%). Adverse events related to EPS occurred in 59.6% of patients treated with haloperidol (n = 99) monotherapy, whereas 26.5% of patients treated with lithium (n = 98) monotherapy experienced adverse events related to EPS. The incidence of akathisia was low and similar with quetiapine monotherapy (3.3%) and placebo (6.1%), and with QTP + Li/DVP (3.6%) and PBO + Li/DVP (4.9%). Lithium was associated with a significantly higher incidence (p < 0.05) of tremor (18.4%) than quetiapine (5.6%); cerebellar tremor, which is a known adverse effect of lithium, may have contributed to the elevated rate of tremor in patients receiving lithium therapy. Haloperidol induced a significantly higher incidence (p < 0.001) of akathisia (33.3% versus 5.9%), tremor (30.3% versus 7.8%), and extrapyramidal syndrome (35.4% versus 5.9%) than quetiapine. No significant differences were observed between quetiapine and placebo on SAS and BARS scores. Anticholinergic use was low and similar with quetiapine or placebo.
CONCLUSIONS
In bipolar mania, the incidence of EPS, including akathisia, with quetiapine therapy is similar to that with placebo.
目的
评估喹硫平治疗双相躁狂症患者时锥体外系症状(EPS),包括静坐不能的情况。
方法
对四项设计相似、随机、双盲、为期3至12周的研究数据进行分析。两项研究评估喹硫平单药治疗(剂量高达800mg/天)(n = 209)与安慰剂(n = 198)对比,分别以锂盐或氟哌啶醇单药治疗作为活性对照。两项研究评估喹硫平(剂量高达800mg/天)联合心境稳定剂(锂盐或丙戊酸,QTP + Li/DVP)(n = 196)与安慰剂联合心境稳定剂(PBO + Li/DVP)(n = 203)对比。使用辛普森-安格斯量表(SAS)、巴恩斯静坐不能评定量表(BARS)、不良事件报告及抗胆碱能药物使用情况来评估锥体外系症状。
结果
包括静坐不能在内的与EPS相关不良事件的发生率,喹硫平单药治疗组(12.9%)与安慰剂组(13.1%)无差异。同样,QTP + Li/DVP组(21.4%)与PBO + Li/DVP组(19.2%)与EPS相关的不良事件无差异。接受氟哌啶醇单药治疗(n = 99)的患者中,59.6%发生了与EPS相关的不良事件,而接受锂盐单药治疗(n = 98)的患者中,26.5%发生了与EPS相关的不良事件。喹硫平单药治疗(3.3%)和安慰剂(6.1%),以及QTP + Li/DVP(3.6%)和PBO + Li/DVP(4.9%)的静坐不能发生率较低且相似。锂盐所致震颤发生率(18.4%)显著高于喹硫平(5.6%)(p < 0.05);小脑震颤是锂盐已知的不良反应,可能导致接受锂盐治疗患者的震颤发生率升高。与喹硫平相比,氟哌啶醇所致静坐不能(33.3% 对5.9%)、震颤(30.3% 对7.8%)和锥体外系综合征(35.4% 对5.9%)发生率显著更高(p < 0.001)。在SAS和BARS评分上,喹硫平与安慰剂之间未观察到显著差异。喹硫平或安慰剂的抗胆碱能药物使用情况较少且相似。
结论
在双相躁狂症中,喹硫平治疗时包括静坐不能在内的EPS发生率与安慰剂相似。
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