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布洛芬缓解牙痛的起始和消退建模。

Modeling the onset and offset of dental pain relief by ibuprofen.

机构信息

Quantitative Solutions Inc, CA 94025, USA.

出版信息

J Clin Pharmacol. 2012 Jan;52(1):89-101. doi: 10.1177/0091270010389470. Epub 2011 Mar 7.

Abstract

Onset and offset of dental pain relief by ibuprofen following third molar extraction were modeled in a randomized, double-blind, placebo-controlled, parallel-group, 8-hour study of patients receiving either a novel effervescent ibuprofen tablet (400 mg; N = 30), standard ibuprofen tablets (Nurofen(®) 2 × 200 mg; N = 22), or placebo (N = 37). An Emax model was fit to pain relief scores. Linear hazard models were used to analyze the time to first perceptible relief (TFPR), the time to meaningful pain relief (TMPR), and time to remedication (REMD). Nomograms were created to correlate TFPR, TMPR, and REMD with different ibuprofen pharmacokinetic profiles. Effervescent ibuprofen was absorbed rapidly with 95% completion within 15 minutes. Maximum pain relief score by ibuprofen was 1.8 units greater than placebo, with an EC50 (effect-site) for ibuprofen concentration of 10.2 µg·mL(-1). The likelihood to achieve TFPR and TMPR was doubled for every 10 µg·mL(-1) increase in ibuprofen plasma concentration. REMD risk decreased 40-fold as the categorical pain relief score increased from 0 to 3. Rapid absorption of ibuprofen effervescent resulted in an earlier TFPR and TMPR, and a lower REMD rate than standard ibuprofen. The nomograms may be useful in predicting the onset and offset of new faster acting ibuprofen formulations, based on pharmacokinetic profiles.

摘要

在一项随机、双盲、安慰剂对照、平行组 8 小时研究中,比较了新型泡腾布洛芬片(400mg;N=30)、标准布洛芬片(Nurofen®2×200mg;N=22)和安慰剂(N=37)用于接受第三磨牙拔除术的患者后,布洛芬对牙痛缓解的起始和消退时间。采用 Emax 模型拟合疼痛缓解评分。线性危险模型用于分析首次可察觉缓解时间(TFPR)、有意义疼痛缓解时间(TMPR)和再次用药时间(REMD)。创建了列线图,以将 TFPR、TMPR 和 REMD 与不同的布洛芬药代动力学特征相关联。泡腾布洛芬的吸收迅速,95%的吸收在 15 分钟内完成。布洛芬的最大疼痛缓解评分比安慰剂高 1.8 个单位,其 EC50(效应部位)的布洛芬浓度为 10.2μg·mL(-1)。布洛芬血浆浓度每增加 10μg·mL(-1),达到 TFPR 和 TMPR 的可能性就会增加一倍。随着疼痛缓解评分从 0 增加到 3,REMD 风险降低了 40 倍。布洛芬泡腾片的快速吸收导致 TFPR 和 TMPR 更早出现,而 REMD 率更低。这些列线图可能有助于预测新型更快起效的布洛芬制剂的起始和消退时间,这取决于药代动力学特征。

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