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首页> 外文期刊>International clinical psychopharmacology >Dose correspondence between olanzapine long-acting injection and oral olanzapine: recommendations for switching.
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Dose correspondence between olanzapine long-acting injection and oral olanzapine: recommendations for switching.

机译:奥氮平长效注射剂与口服奥氮平之间的剂量对应:转换建议。

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摘要

Oral-to-depot dose correspondence was explored in a 24-week study of olanzapine long-acting injection (LAI). Patients with schizophrenia stabilized on oral olanzapine of 10, 15, or 20 mg/day (n=1065) were randomized to continue their oral treatment or switch directly to a fixed dose of olanzapine LAI [(mg/weeks) 45/4, 150/2, 405/4, or 300/2] without oral supplementation. Six-month relapse rates for each LAI-dose group stratified by earlier oral dose were analyzed using a Cox proportional hazard model assessing risk of relapse relative to each oral dose. Relapse rates for the therapeutic LAI doses (>/= 150 mg) varied depending on earlier oral dose, ranging from 1.5% (patients switched from 10 mg/day to 300 mg/2 weeks) to 18.8% (patients switched from 20 mg/day to 150 mg/2 weeks). Switching from 10 mg/day to 405 mg/4 weeks produced a comparable risk of relapse as remaining on that oral dose [Hazard ratio (HR)=1.03]. Switching from 15 or 20 mg/day to 300 mg/2 weeks produced comparable risk of relapse as remaining on those oral doses (HR=0.68 and 1.13, respectively). Pharmacokinetic modeling was conducted to evaluate the resulting dosing recommendations. Findings suggest that patients can be switched directly from oral to olanzapine LAI without the need for oral supplementation and with a low risk of relapse when initiated on an appropriate LAI dose.
机译:在奥氮平长效注射剂(LAI)的24周研究中探讨了口服至口服剂量的对应关系。每天口服10、15或20 mg奥氮平稳定的精神分裂症患者(n = 1065)被随机分配以继续口服治疗或直接改用固定剂量的olanzapine LAI [(mg / weeks)45/4,150 / 2、405 / 4或300/2],而无需口服补充剂。通过评估相对于每个口服剂量的复发风险的Cox比例风险模型,对按早期口服剂量分层的每个LAI剂量组的六个月复发率进行了分析。治疗性LAI剂量(> / = 150 mg)的复发率取决于早期口服剂量,范围从1.5%(患者从10 mg /天转换为300 mg / 2周)到18.8%(患者从20 mg /一天至150 mg / 2周)。从10毫克/天转换为405毫克/ 4周可产生与口服剂量相同的复发风险[危险比(HR)= 1.03]。从15或20毫克/天转换为300毫克/ 2周产生的复发风险与那些口服剂量相同(分别为HR = 0.68和1.13)。进行了药代动力学建模以评估最终的剂量建议。研究结果表明,患者可以直接从口服LAI转换为奥氮平LAI,而无需口服补充剂,并且以适当的LAI剂量启动后复发风险低。

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