External evaluation of intravenous vancomycin population pharmacokinetic models in adults receiving high-flux intermittent haemodialysis

IF 3.1 3区医学 Q2 PHARMACOLOGY & PHARMACY

British journal of clinical pharmacology Pub Date : 2024-11-09 DOI:10.1111/bcp.16334

Cheng Ji, Jonathan Garcia, Argem Joy Sabuga, Maurane Ricard, France Dion, Vlad Alexandru Rosu, Marie-Ève Legris, Amélie Marsot, Van Dong Nguyen

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引用次数: 0

Abstract

Aims

Patients undergoing haemodialysis (HD) are at greater risk of methicillin-resistant Staphylococcus aureus infections requiring intravenous vancomycin. Close vancomycin therapeutic drug monitoring is warranted in HD patients as renal clearance is the primary elimination pathway. Clinically, population pharmacokinetics (popPK) model-informed dosing is commonly used. This study aimed to perform an external evaluation of published vancomycin popPK models developed for adults undergoing high-flux intermittent HD, and to create a dosing nomogram derived from the model that performed best.

Methods

A literature review was conducted through PubMed and EMBASE to identify relevant popPK models. an external dataset was collected retrospectively from patients of 2 healthcare centres in Quebec, Canada. Selected models were implemented in NONMEM (v7.5; ICON Development Solutions). Predictive performance was assessed through prediction and simulation-based diagnostics.

Results

In total, 2386 vancomycin concentrations were collected from 274 patients and 476 antibiotic courses. Four vancomycin popPK models were selected for evaluation. None of the models demonstrated overall satisfactory or clinically acceptable predictive performance. Nonetheless, Bae et al.’s model performed best with a median prediction error of 16.25% and median absolute prediction error of 34.66%. Different predictive performance was also observed for vancomycin concentrations from samples collected during and between HD sessions.

Conclusion

All evaluated models presented poor overall predictive performance. Further studies are required, through existing popPK model parameter re-estimation or new model development, to adequately describe vancomycin pharmacokinetics for our high-flux intermittent HD patient cohort.

Abstract Image

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对接受高通量间歇性血液透析的成人静脉注射万古霉素群体药代动力学模型进行外部评估。

目的：接受血液透析（HD）的患者发生耐甲氧西林金黄色葡萄球菌感染的风险更大，需要静脉注射万古霉素。由于肾脏清除是消除万古霉素的主要途径，因此需要对血液透析患者进行密切的万古霉素治疗药物监测。临床上通常使用群体药代动力学（popPK）模型指导用药。本研究旨在对已发表的万古霉素流行药代动力学模型进行外部评估，这些模型是为接受高通量间歇性 HD 治疗的成人开发的，并根据表现最佳的模型创建了一个剂量提名图：通过 PubMed 和 EMBASE 进行文献综述，以确定相关 popPK 模型。选定的模型在 NONMEM（v7.5；ICON Development Solutions）中实施。通过预测和模拟诊断评估了预测性能：总共从 274 名患者和 476 个抗生素疗程中收集到 2386 个万古霉素浓度。我们选择了四个万古霉素 popPK 模型进行评估。这些模型均未显示出令人满意或临床可接受的整体预测性能。不过，Bae 等人的模型表现最好，预测误差中位数为 16.25%，绝对预测误差中位数为 34.66%。对于在血液透析过程中和两次透析之间采集的样本中的万古霉素浓度，也观察到了不同的预测性能：结论：所有评估模型的总体预测性能都较差。结论：所有评估模型的总体预测性能较差，需要通过现有 popPK 模型参数的重新估计或新模型的开发进行进一步研究，以充分描述高流量间歇性 HD 患者队列的万古霉素药代动力学。

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

British journal of clinical pharmacology 医学-药学

CiteScore

6.30

自引率

8.80%

发文量

419

审稿时长

1 months

期刊介绍： Published on behalf of the British Pharmacological Society, the British Journal of Clinical Pharmacology features papers and reports on all aspects of drug action in humans: review articles, mini review articles, original papers, commentaries, editorials and letters. The Journal enjoys a wide readership, bridging the gap between the medical profession, clinical research and the pharmaceutical industry. It also publishes research on new methods, new drugs and new approaches to treatment. The Journal is recognised as one of the leading publications in its field. It is online only, publishes open access research through its OnlineOpen programme and is published monthly.