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洛匹那韦药代动力学中体重相关差异的人群分析及其对初治和经治蛋白酶抑制剂患者的可能影响。

A population analysis of weight-related differences in lopinavir pharmacokinetics and possible consequences for protease inhibitor-naive and -experienced patients.

作者信息

Bouillon-Pichault Marion, Jullien Vincent, Piketty Christophe, Viard Jean-Paul, Morini Jean-Pierre, Chhun Stéphanie, Krivine Anne, Salmon Dominique, Dupin Nicolas, Weiss Laurence, Lortholary Olivier, Pons Gérard, Launay Odile, Treluyer Jean-Marc

机构信息

Université Paris Descartes, Paris, France.

出版信息

Antivir Ther. 2009;14(7):923-9. doi: 10.3851/IMP1414.

DOI:10.3851/IMP1414
PMID:19918096
Abstract

BACKGROUND

Lopinavir is a potent protease inhibitor (PI) used for the treatment of HIV infection. Different lopinavir target trough concentrations (C(troughs)) were previously determined according to patient treatment histories: 1 mg/l for PI-naive patients, and 4 and 5.7 mg/l for PI-experienced patients. However, the probability to achieve these target C(troughs) with the current 400 mg twice-daily or 800 mg once-daily doses of the new tablet form, and the influence of body weight on this probability are unknown.

METHODS

A population pharmacokinetic model for lopinavir was developed using data from 424 HIV type-1-infected patients, and the final model was used to estimate the probability to achieve target C(troughs) via Monte Carlo simulations.

RESULTS

A one-compartment model adequately described the data. Mean population estimates (percentage interindividual variability) were 4.61 l/h (36%) for apparent clearance (CL/F) and 63.2 l (70%) for apparent distribution volume. Body weight was found to explain the interindividual variability of lopinavir CL/F. Probability to achieve the 1 mg/l target C(trough) was >96% for the twice-daily dose and comprised between 80% and 90% for the once-daily dose. The probability to achieve the 4 and 5.7 mg/l target C(troughs) with the twice-daily dose significantly decreased when body weight increased (from 76% to 61% and from 56% to 37% respectively, for body weights increasing from 50 to 90 kg).

CONCLUSIONS

These results support lopinavir therapeutic drug monitoring and the use of higher lopinavir doses for PI-pretreated patients.

摘要

背景

洛匹那韦是一种用于治疗HIV感染的强效蛋白酶抑制剂(PI)。先前根据患者治疗史确定了不同的洛匹那韦目标谷浓度(C谷):初治PI患者为1mg/L,经治PI患者为4mg/L和5.7mg/L。然而,使用新片剂形式的当前每日两次400mg或每日一次800mg剂量达到这些目标C谷的概率,以及体重对该概率的影响尚不清楚。

方法

利用424例HIV-1感染患者的数据建立了洛匹那韦的群体药代动力学模型,并使用最终模型通过蒙特卡洛模拟估计达到目标C谷的概率。

结果

单室模型充分描述了数据。表观清除率(CL/F)的群体平均估计值(个体间变异百分比)为4.61L/h(36%),表观分布容积为63.2L(70%)。发现体重可解释洛匹那韦CL/F的个体间变异。每日两次给药达到1mg/L目标C谷的概率>96%,每日一次给药的概率在80%至90%之间。当体重增加时,每日两次给药达到4mg/L和5.7mg/L目标C谷的概率显著降低(体重从50kg增加到90kg时,分别从76%降至61%和从56%降至37%)。

结论

这些结果支持洛匹那韦的治疗药物监测以及对PI预处理患者使用更高剂量的洛匹那韦。

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