Individualization of piperacillin dosage based on therapeutic drug monitoring with or without model-informed precision dosing: a scenario analysis.

IF 3.9 2区 医学 Q1 INFECTIOUS DISEASES Journal of Antimicrobial Chemotherapy Pub Date : 2025-01-17 DOI:10.1093/jac/dkaf007
David Haefliger, Lynn Mina, Monia Guidi, Catia Marzolini, Paul Thoueille, Laura E Rothuizen, Yann Thoma, Laurent A Decosterd, Benoit Guery, François R Girardin, Thierry Buclin
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Abstract

Background: Model-informed precision dosing (MIPD) combines population pharmacokinetic knowledge with therapeutic drug monitoring (TDM) to optimize dosage adjustment. It could improve target concentration attainment over empirical TDM, still widely practised for broad-spectrum antibiotics.

Objectives: To evaluate the respective performance of TDM and MIPD in achieving target piperacillin exposure.

Methods: Measurements from 80 courses of intermittent piperacillin infusions, each with two TDM samples, were retrospectively submitted to our MIPD software TUCUXI. We considered six dosage adjustment strategies: identical dosage for all (4000 mg q8h), actual initial dosage (chart-based), actual empirical adjustment following first TDM, a priori MIPD-based dosage, a posteriori MIPD-based adjustment after first TDM and MIPD including both TDM measurements. Dosing strategies were compared regarding daily dosage, trough levels distribution and PTA (with target trough 8-32 mg/L).

Results: Median trough concentration fell within 8-32 mg/L for all strategies except a priori MIPD-based dosage (42 mg/L). Distributions of trough concentrations predicted with the six dosage adjustment strategies showed significant differences, with both a posteriori MIPD-based strategies best reducing their standard deviation (P < 0.001). PTA of 32%, 32%, 55%, 29%, 83% and 94% were estimated, respectively for the six strategies (P < 0.001). Poor performance of a priori MIPD-based dosage did not hinder a posteriori MIPD-based strategies from significantly improving target attainment.

Conclusions: Whilst empirical TDM improves exposure standardization and target attainment compared with no TDM, MIPD can still bring further improvement. Prospective trials remain warranted to confirm MIPD benefits not only on target attainment but also on clinical endpoints.

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基于治疗药物监测的哌拉西林个体化剂量,有或没有模型信息的精确给药:情景分析。
背景:基于模型的精确给药(MIPD)将人群药代动力学知识与治疗药物监测(TDM)相结合,以优化剂量调整。与经验性TDM相比,它可以提高目标浓度,目前仍广泛应用于广谱抗生素。目的:评价TDM和MIPD在实现哌拉西林靶暴露中的各自表现。方法:回顾性地将80个疗程的间歇性哌拉西林输注的测量结果提交到我们的MIPD软件TUCUXI中,每个疗程有两个TDM样本。我们考虑了六种剂量调整策略:所有人的相同剂量(4000 mg q8h),实际初始剂量(基于图表),首次TDM后的实际经验调整,先验的基于MIPD的剂量,首次TDM后基于MIPD的后验调整和MIPD包括两种TDM测量。比较两组给药策略的日给药量、波谷分布和PTA(目标波谷8 ~ 32mg /L)。结果:除基于mipd的先验剂量(42 mg/L)外,所有策略的中位谷浓度均在8-32 mg/L范围内。6种剂量调整策略预测的谷浓度分布存在显著差异,基于后验MIPD的两种策略均能最大程度地降低其标准差(P)。结论:虽然与不采用TDM相比,经经验TDM能提高暴露标准化和目标达成程度,但MIPD仍能进一步改善。前瞻性试验仍有必要确认MIPD不仅在目标实现上而且在临床终点上的益处。
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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来源期刊
CiteScore
9.20
自引率
5.80%
发文量
423
审稿时长
2-4 weeks
期刊介绍: The Journal publishes articles that further knowledge and advance the science and application of antimicrobial chemotherapy with antibiotics and antifungal, antiviral and antiprotozoal agents. The Journal publishes primarily in human medicine, and articles in veterinary medicine likely to have an impact on global health.
期刊最新文献
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