马体内苄青霉素的药代动力学-药效学截断值,用于支持建立马的苄青霉素抗菌药物敏感性试验的临床断点。
Pharmacokinetic-pharmacodynamic cutoff values for benzylpenicillin in horses to support the establishment of clinical breakpoints for benzylpenicillin antimicrobial susceptibility testing in horses.
作者信息
Lallemand Elodie A, Bousquet-Mélou Alain, Chapuis Laura, Davis Jennifer, Ferran Aude A, Kukanich Butch, Kuroda Taisuke, Lacroix Marlène Z, Minamijima Yohei, Olsén Lena, Pelligand Ludovic, Portugal Felipe Ramon, Roques Béatrice B, Santschi Elizabeth M, Wilson Katherine E, Toutain Pierre-Louis
机构信息
INTHERES, Université de Toulouse, INRAE, ENVT, Toulouse, France.
Department of Biomedical Sciences and Pathobiology, Virginia-Maryland College of Veterinary Medicine, Blacksburg, VA, United States.
出版信息
Front Microbiol. 2023 Oct 25;14:1282949. doi: 10.3389/fmicb.2023.1282949. eCollection 2023.
INTRODUCTION
The aim of this international project was to establish a species-specific Clinical Breakpoint for interpretation of Antimicrobial Susceptibility Testing of benzylpenicillin (BP) in horses.
METHODS
A population pharmacokinetic model of BP disposition was developed to compute PK/PD cutoff values of BP for different formulations that are commonly used in equine medicine around the world (France, Sweden, USA and Japan). Investigated substances were potassium BP, sodium BP, procaine BP, a combination of procaine BP and benzathine BP and penethamate, a prodrug of BP. Data were collected from 40 horses that provided 63 rich profiles of BP corresponding to a total of 1022 individual BP plasma concentrations.
RESULTS
A 3-compartment disposition model was selected. For each of these formulations, the PK/PD cutoff was estimated for different dosage regimens using Monte Carlo simulations. The AUC/MIC or T>MIC were calculated with a free BP fraction set at 0.4. For AUC/MIC, a target value of 72 h (for a 72h treatment) was considered. For T>MIC, efficacy was assumed when free plasma concentrations were above the explored MIC (0.0625-2 mg/L) for 30 or 40 % of the dosing interval. For continuous infusion, a T>MIC of 90 % was considered. It was shown that a PK/PD cutoff of 0.25 mg/L can be achieved in 90 % of horses with routine regimen (typically 22,000 IU/kg or 12.4 mg/kg per day) with IM procaine BP once a day (France, Japan, Sweden but not USA1) and with IM sodium BP at 14.07 mg/kg, twice a day or IV sodium BP infusion of 12.4 mg/kg per day. In contrast, penethamate and the combination of procaine BP and benzathine BP were unable to achieve this PK/PD cutoff not even an MIC of 0.125 mg/L.
DISCUSSION
The PK/PD cutoff of 0.25 mg/L is one dilution lower than the clinical breakpoint released by the CLSI (0.5 mg/ L). From our simulations, the CLSI clinical breakpoint can be achieved with IM procaine BP twice a day at 22,000 IU i.e. 12.4 mg/kg.
引言
这个国际项目的目的是建立一个物种特异性的临床断点,用于解释马匹中苄青霉素(BP)的抗菌药敏试验结果。
方法
建立了BP处置的群体药代动力学模型,以计算全球马匹医学中常用的不同制剂(法国、瑞典、美国和日本)的BP的PK/PD截止值。研究的物质包括BP钾盐、BP钠盐、普鲁卡因BP、普鲁卡因BP和苄星BP的组合以及BP的前体药物戊四氮。数据收集自40匹马,这些马提供了63个丰富的BP曲线,对应总共1022个个体BP血浆浓度。
结果
选择了三室处置模型。对于这些制剂中的每一种,使用蒙特卡洛模拟估计了不同给药方案的PK/PD截止值。AUC/MIC或T>MIC是在游离BP分数设定为0.4的情况下计算的。对于AUC/MIC,考虑了72小时(对于72小时治疗)的目标值。对于T>MIC,当游离血浆浓度在给药间隔的30%或40%高于探索的MIC(0.0625 - 2 mg/L)时,假设有效。对于持续输注,考虑T>MIC为90%。结果表明,对于法国、日本、瑞典(但美国不行)每天一次肌肉注射普鲁卡因BP的常规方案(通常为22,000 IU/kg或12.4 mg/kg/天)以及每天两次14.07 mg/kg肌肉注射BP钠盐或每天12.4 mg/kg静脉输注BP钠盐,90%的马匹可以达到0.25 mg/L的PK/PD截止值。相比之下,戊四氮以及普鲁卡因BP和苄星BP的组合甚至无法达到0.125 mg/L的MIC,更无法达到这个PK/PD截止值。
讨论
0.25 mg/L的PK/PD截止值比CLSI发布的临床断点(0.5 mg/L)低一个稀释度。从我们的模拟来看,每天两次22,000 IU即12.4 mg/kg肌肉注射普鲁卡因BP可以达到CLSI临床断点。
Zotero 插件