The pharmacokinetic profile of a novel fixed-dose combination tablet of ibuprofen and paracetamol.

Trevor Tanner, Sue Aspley, Andrew Munn, Tracy Thomas
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引用次数: 46

Abstract

Background: Ibuprofen and paracetamol differ in their mode of action and related therapeutic effects, suggesting that combined administration may offer improved analgesia. Reported here are the results of two studies on the pharmacokinetic properties of a novel ibuprofen (200 mg) and paracetamol (500 mg) fixed-dose combination tablet.

Methods: Both studies were open-label, randomised studies in healthy volunteers: Study 1 was a four-way crossover, single-dose study; Study 2 was a two-way cross-over, repeat-dose study.

Results: Pharmacokinetic parameters for ibuprofen and paracetamol were similar for the combination and monotherapy tablets (values falling within the 80% to 125% acceptable bioequivalence range) except for the rate of absorption of paracetamol from the combination (tmax), which was significantly faster compared with monotherapy (median difference 10 minutes; p < 0.05). Mean plasma concentrations of both drugs were higher, earlier, following administration of the combination tablet compared with monotherapy. Mean plasma levels at 10 and 20 minutes were 6.64 microg x mL(-1) and 16.81 microg x mL(-1), respectively, for ibuprofen from the combination, compared with 0.58 microg x mL(-1) and 9.00 microg x mL-1, respectively, for monotherapy. For paracetamol, mean plasma levels at 10 and 20 minutes were 5.43 microg x mL(-1) and 14.54 microg x mL(-, respectively, for the combination compared with 0.33 microg x mL(-1) and 9.19 microg x mL(-1), respectively, for monotherapy. The rate of absorption of both ibuprofen and paracetamol was significantly delayed when the combination tablet was administered in the fed versus fasted state; median delay was 25 minutes for ibuprofen (p > 0.05) and 55 minutes for paracetamol (p < 0.001). The pharmacokinetic parameters were comparable irrespective of whether the combination tablet was given twice or three times daily; systemic exposure was, however, approximately 1.4 times greater for both drugs when given three times daily.

Conclusions: Administration of ibuprofen and paracetamol in a fixed-dose combination tablet does not significantly alter the pharmacokinetic profiles of either drug, except for enhancing the rate of paracetamol absorption, offering potential therapeutic benefits in relation to the onset of analgesia. Concentrations of both drugs reached previously reported therapeutic levels when the combination tablet was administrated in the fed or fasted state. Three times daily dosing may offer enhanced therapeutic effect for longer than twice daily dosing.

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一种新型布洛芬和扑热息痛固定剂量联用片的药代动力学特征。
背景:布洛芬和扑热息痛的作用方式和相关治疗效果不同,提示联合用药可改善镇痛效果。本文报道了一种新型布洛芬(200 mg)和扑热息痛(500 mg)固定剂量复合片的药代动力学特性的两项研究结果。方法:两项研究均为在健康志愿者中进行的开放标签、随机化研究:研究1为四向交叉、单剂量研究;研究2是一项双向交叉、重复给药研究。结果:布洛芬和扑热息痛的药代动力学参数与单药片相似(均在80% ~ 125%可接受生物等效性范围内),但对扑热息痛的吸收速率(tmax)明显快于单药片(中位差10分钟;P < 0.05)。与单药治疗相比,联合用药后两种药物的平均血浆浓度更高,更早。联合布洛芬组10分钟和20分钟的平均血浆水平分别为6.64 μ g × mL(-1)和16.81 μ g × mL(-1),而单药组分别为0.58 μ g × mL(-1)和9.00 μ g × mL-1。对于扑热息痛,联合用药10分钟和20分钟的平均血浆水平分别为5.43 μ g × mL(-1)和14.54 μ g × mL(-1),而单药治疗分别为0.33 μ g × mL(-1)和9.19 μ g × mL(-1)。布洛芬和扑热息痛的吸收率在进食和禁食状态下均显著延迟;布洛芬组的中位延迟为25分钟(p > 0.05),扑热息痛组的中位延迟为55分钟(p < 0.001)。无论复方片每日服用2次还是3次,其药代动力学参数均具有可比性;然而,当每天给药三次时,两种药物的全身暴露量约为1.4倍。结论:布洛芬和扑热息痛在固定剂量联合片剂中服用,除了提高扑热息痛的吸收率外,没有显著改变两种药物的药代动力学特征,与镇痛发作有关,提供了潜在的治疗益处。两种药物的浓度达到先前报道的治疗水平,当联合片剂在进食或禁食状态下给予。每日三次给药比每日两次给药时间更长,可提供增强的治疗效果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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