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奥氮平:其用于治疗双相I型障碍的综述。

Olanzapine: a review of its use in the treatment of bipolar I disorder.

作者信息

Bhana N, Perry C M

机构信息

Adis International Limited, Auckland, New Zealand.

出版信息

CNS Drugs. 2001;15(11):871-904. doi: 10.2165/00023210-200115110-00005.

Abstract

UNLABELLED

Olanzapine, a thienobenzodiazepine derivative, is a psychotropic agent that has shown efficacy in the treatment of patients with bipolar I disorder. Olanzapine has a multireceptorial binding profile including a greater affinity for serotonin 5-HT(2A) than for dopamine D(2) receptors. Olanzapine 5 to 20 mg/day demonstrated significantly greater antimanic efficacy than placebo in two double-blind, randomised 3- or 4-week trials of patients with bipolar I disorder of either manic or mixed episodes, with or without psychotic features. Additionally, in one of these trials, improvements in cognitive function and hostility were superior with olanzapine. In cohorts of severely depressed and rapid cycling patients, improvements in manic and depressive symptoms and in manic symptoms only, were superior with olanzapine compared with placebo. Significant improvements from baseline in symptoms of mania, depression, cognitive functioning and hostility were seen with olanzapine in a 49-week extension phase study. In double-blind trials, olanzapine 10 mg/day appeared to have similar antimanic efficacy to oral lithium 400mg twice daily in the treatment of patients with pure mania (4-week small study). In patients with acute manic or mixed episodes olanzapine 5 to 20 mg/day appeared to be more effective than oral valproate semisodium (divalproex sodium) 500 to 2500 mg/day (3-week study) and at least as effective as oral haloperidol 3 to 15 mg/day (12-week study). Preliminary results from a large 6-week placebo-controlled study suggest that olanzapine 5 to 20 mg/day in combination with mood stabilisers (lithium or valproate semisodium) provides effective augmentation of antimanic treatment of patients with bipolar I disorder, with benefits seen in the first week. Adverse events reported significantly more often with olanzapine than with placebo were somnolence, dry mouth, dizziness and bodyweight gain, and in comparison with valproate semisodium were somnolence, dry mouth, increased appetite and bodyweight gain. Olanzapine was generally well tolerated with no clinically relevant abnormalities in laboratory tests, vital signs or electrocardiogram results.

CONCLUSION

Olanzapine demonstrated superior efficacy compared with placebo in the short-term treatment of patients with bipolar I disorder with manic or mixed episodes, with or without psychotic features, and was generally well tolerated. According to preliminary data the antimanic efficacy of olanzapine appears similar to that of haloperidol and better than that of valproate semisodium in patients with bipolar I disorder experiencing a manic or mixed episode; among nonpsychotic patients with manic or mixed episodes olanzapine appears to be superior to haloperidol. Available data support the choice of olanzapine as an option in the short-term management of mania in patients with bipolar I disorder with manic or mixed episodes, with or without psychotic features.

摘要

未标注

奥氮平是一种噻吩并苯二氮䓬衍生物,是一种精神药物,已显示出对双相I型障碍患者的治疗效果。奥氮平具有多受体结合特征,对5-羟色胺5-HT(2A)的亲和力高于多巴胺D(2)受体。在两项针对双相I型障碍躁狂或混合发作患者(有或无精神病性特征)的双盲、随机3或4周试验中,奥氮平5至20毫克/天的抗躁狂疗效显著优于安慰剂。此外,在其中一项试验中,奥氮平在改善认知功能和敌意方面更具优势。在重度抑郁和快速循环患者队列中,与安慰剂相比,奥氮平在改善躁狂和抑郁症状以及仅改善躁狂症状方面更具优势。在一项49周的延长期研究中,奥氮平使躁狂、抑郁、认知功能和敌意症状较基线有显著改善。在双盲试验中,奥氮平10毫克/天在治疗单纯躁狂患者(4周小型研究)时,其抗躁狂疗效似乎与每日两次口服400毫克锂盐相似。在急性躁狂或混合发作患者中,奥氮平5至20毫克/天似乎比口服丙戊酸半钠(丙戊酸钠)500至2500毫克/天更有效(3周研究),且至少与口服氟哌啶醇3至15毫克/天效果相当(12周研究)。一项为期6周的大型安慰剂对照研究的初步结果表明,奥氮平5至20毫克/天与心境稳定剂(锂盐或丙戊酸半钠)联合使用,可有效增强双相I型障碍患者的抗躁狂治疗效果,且在第一周即可见到疗效。与安慰剂相比,奥氮平报告的不良事件明显更多的是嗜睡、口干、头晕和体重增加,与丙戊酸半钠相比则是嗜睡、口干、食欲增加和体重增加。奥氮平总体耐受性良好,实验室检查、生命体征或心电图结果均无临床相关异常。

结论

与安慰剂相比,奥氮平在短期治疗双相I型障碍躁狂或混合发作患者(有或无精神病性特征)方面显示出更优的疗效,且总体耐受性良好。根据初步数据,在双相I型障碍躁狂或混合发作患者中,奥氮平的抗躁狂疗效似乎与氟哌啶醇相似,且优于丙戊酸半钠;在无精神病性特征的躁狂或混合发作患者中,奥氮平似乎优于氟哌啶醇。现有数据支持选择奥氮平作为双相I型障碍躁狂或混合发作患者(有或无精神病性特征)短期躁狂管理的一种选择。

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