Population pharmacokinetics of colistin sulfate in patients on continuous veno-venous hemodiafiltration.

IF 2.6 4区综合性期刊 Q2 MULTIDISCIPLINARY SCIENCES

Science Progress Pub Date : 2025-01-01 DOI:10.1177/00368504251325334

Tianmin Huang, Yilin Luo, Yun Wu, Lulu Niu, Yang Xiao, Tingqing Wu, Xin Chen, Yongjun Liu, Jiejiu Lu, Donglan Zhu, Taotao Liu

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引用次数: 0

Abstract

Objective: The aim of this study is to establish a population pharmacokinetic (PK) model for patients undergoing continuous veno-venous hemodiafiltration (CVVHDF) and optimize the dosing regimen of colistin sulfate.

Methods: A prospective observational study in a single center was conducted on patients who were administrated with colistin sulfate and CVVHDF for at least 48 h. Blood samples were obtained prior to dosing and four to six blood samples (primarily C_0.5h, C_1h, C_2h, C_4h, and C_6h) after dosing. The blood concentration of colistin sulfate was determined by ultra-high performance liquid chromatography-tandem mass spectrometry assay. The NONMEM program was used to establish the population PK model and perform Monte Carlo simulations. The predictability and stability of the model were internally evaluated by the goodness of fit plots, visual prediction check, and bootstraps.

Results: A total of 86 plasma concentrations from 20 patients were used for population PK modeling. A two-compartment model with first-order linear elimination best described the population PK characteristics of colistin sulfate. Cystatin C (CysC) and body weight (WT) were identified as covariates for clearance (CL). Internal evaluation results showed that the final model had good stability and prediction performance. Monte Carlo simulations showed that only when the body WT was 50 kg with CysC ≥3.07 mg/l, and when the body WT was 65 kg with CysC = 5.11 mg/l, and minimum inhibitory concentration (MIC) = 0.25 mg/l, the target attainment probability (PTA) of the daily dose of 1.5 million U regimen was ≥90%. All treatment regimens fail to achieve the target PTA when MIC = 1 mg/l.

Conclusions: With the decrease of CysC levels and the increase of WT, the dose of colistin sulfate may need to be increased. It may be prudent for colistin sulfate to consider an initial dose doubling and subsequent maintenance dosing regimen of 200-225 million unit daily, administered in 2-3 divided doses, to attain PTA standard. This study was registered at the Chinese Clinical Trial Registry (www.chictr.org.cn) (trial registration number ChiCTR2300072191).

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持续静脉-静脉血液渗滤患者硫酸粘菌素的人群药代动力学。

目的：建立连续静脉-静脉血液渗滤（CVVHDF）患者的群体药代动力学（PK）模型，优化硫酸粘菌素给药方案。方法：在单中心对给予硫酸粘菌素和CVVHDF至少48小时的患者进行前瞻性观察研究。给药前采集血样，给药后采集4 - 6份血样（主要是C0.5h、C1h、C2h、C4h和C6h）。采用超高效液相色谱-串联质谱法测定硫酸粘菌素血药浓度。利用NONMEM程序建立种群PK模型，并进行蒙特卡罗模拟。模型的可预测性和稳定性通过拟合优度、视觉预测检查和自举进行内部评估。结果：20例患者共86个血浆浓度用于群体PK模型。一阶线性消除的双室模型最能描述硫酸粘菌素的种群PK特性。Cystatin C （CysC）和体重（WT）被确定为清除率（CL）的协变量。内部评价结果表明，最终模型具有良好的稳定性和预测性能。Monte Carlo模拟表明，只有当体WT为50 kg， CysC≥3.07 mg/l，体WT为65 kg， CysC = 5.11 mg/l，最小抑制浓度(MIC) = 0.25 mg/l时，150万U方案日剂量的目标实现概率(PTA)≥90%。当MIC = 1 mg/l时，所有治疗方案均不能达到目标PTA。结论：随着CysC水平的降低和WT的增加，可能需要增加硫酸粘菌素的剂量。对于硫酸粘菌素，为达到PTA标准，可考虑初始剂量加倍，随后维持每日2- 2.25亿单位的给药方案，分2-3次给药。本研究已在中国临床试验注册中心（www.chictr.org.cn）注册（试验注册号ChiCTR2300072191）。

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

Science Progress Multidisciplinary-Multidisciplinary

CiteScore

3.80

自引率

0.00%

发文量

119

期刊介绍： Science Progress has for over 100 years been a highly regarded review publication in science, technology and medicine. Its objective is to excite the readers'' interest in areas with which they may not be fully familiar but which could facilitate their interest, or even activity, in a cognate field.