Simpson George M, O'Gorman Cedric J, Loebel Antony, Yang Ruoyong
Department of Psychiatry and the Behavioral Sciences, Keck School of Medicine-University of Southern California, Los Angeles, CA, USA.
CNS Spectr. 2008 Oct;13(10):898-905. doi: 10.1017/s1092852900017004.
The long-term efficacy and tolerability of treatment with ziprasidone following a switch from prior antipsychotics was evaluated in outpatients with schizophrenia or schizoaffective disorder in three open-label, flexible-dose, 1-year extension studies.
These studies enrolled completers of 6-week trials in which subjects were switched to ziprasidone from conventional antipsychotics, olanzapine, or risperidone. Identical study designs and the small number of patients entering the extensions supported pooling of the data.
Of 185 pooled subjects entering the extension studies, 72 completed 58 weeks of treatment. Median treatment duration was 34.6 weeks; median dose was 120 mg/day at endpoint. The intent-to-treat population showed significant improvement in Positive and Negative Syndrome Scale (PANSS) total scores (-4.3 [P< or =.01]), PANSS negative scores (-2.4 [P< or =.0001]), and Clinical Global Impression of severity score (-0.3 [P< or =.001]). Completers showed significant improvement in mean PANSS total scores (-10.2 [P<.0001]), PANSS positive scores (-2.7 [P< .0001]), PANSS negative scores (-2.7 [P< .001]), and Clinical Global Impression of severity scores (-0.6 [P< .0001]).
Ziprasidone was well tolerated, and patients demonstrated significant improvement in metabolic parameters and in all movement disorder assessments. Insomnia and somnolence were the only adverse events with an incidence >10% in pooled subjects. No subject had a corrected QT interval > or =500 msec.
在三项开放标签、灵活剂量、为期1年的延长期研究中,对患有精神分裂症或分裂情感性障碍的门诊患者从先前抗精神病药物换用齐拉西酮治疗后的长期疗效和耐受性进行了评估。
这些研究纳入了为期6周试验的完成者,在这些试验中,受试者从传统抗精神病药物、奥氮平或利培酮换用齐拉西酮。相同的研究设计以及进入延长期的患者数量较少支持了数据合并。
在进入延长期研究的185名合并受试者中,72名完成了58周的治疗。中位治疗持续时间为34.6周;终点时中位剂量为120毫克/天。意向性治疗人群在阳性和阴性症状量表(PANSS)总分(-4.3 [P≤0.01])、PANSS阴性评分(-2.4 [P≤0.0001])和临床总体印象严重程度评分(-0.3 [P≤0.001])方面有显著改善。完成者在平均PANSS总分(-10.2 [P<0.0001])、PANSS阳性评分(-2.7 [P<0.0001])、PANSS阴性评分(-2.7 [P<0.001])和临床总体印象严重程度评分(-0.6 [P<0.0001])方面有显著改善。
齐拉西酮耐受性良好,患者在代谢参数和所有运动障碍评估方面均有显著改善。失眠和嗜睡是合并受试者中仅有的发生率>10%的不良事件。没有受试者的校正QT间期≥500毫秒。
