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固定剂量与基于体重的达托霉素给药策略可能改善肥胖成年人的安全性。

A Fixed versus Weight-Based Dosing Strategy of Daptomycin May Improve Safety in Obese Adults.

机构信息

HealthTrust Supply Chain, Richmond, Virginia.

Albany College of Pharmacy and Health Sciences, Albany, New York.

出版信息

Pharmacotherapy. 2018 Sep;38(9):981-985. doi: 10.1002/phar.2157. Epub 2018 Jul 12.

DOI:10.1002/phar.2157
PMID:29906315
Abstract

OBJECTIVES

To compare daptomycin exposures and predicted safety outcomes with a simulated weight-based and fixed dose in morbidly obese and nonobese subjects.

METHODS

We performed a nonparametric population pharmacokinetic analysis of daptomycin concentration-time data from a prior obese and nonobese kidney function-matched cohort of healthy adult volunteers. Monte Carlo simulations were performed to compare the maximum concentrations (C ), minimum concentrations (C ), and area under the curve (AUC) with the standard daptomycin 6 mg/kg/day dose or a 500-mg daily fixed dose in obese and nonobese subjects. The probability of exceeding a daptomycin C target (24.3 mg/L or higher) associated with creatine phosphokinase (CPK) elevations was computed with the two regimens.

RESULTS

No significant differences were observed in clearance, volume of distribution at steady state, or terminal half-life between the morbidly obese and nonobese PK models. Daptomycin 6 mg/kg/day resulted in AUC, C , and C values that were ~2-fold higher in morbidly obese subjects relative to nonobese individuals. In contrast, fixed dosing (500 mg/day) resulted in relatively isometric exposures. The fraction of simulated morbidly obese subjects with a C target associated with CPK elevations was 10.8% with 6 mg/kg/day and 2.0% at the 500 mg/day dosage.

CONCLUSIONS

Weight-based maintenance dosing of daptomycin is less likely to yield bioequivalent exposures in morbidly obese subjects and provides credence for the evaluation of fixed maintenance doses across adult body size to improve safety.

摘要

目的

比较基于模拟体重和固定剂量的达托霉素暴露量和预测安全性结果,在病态肥胖和非肥胖受试者中。

方法

我们对先前肥胖和非肥胖肾功能匹配的健康成年志愿者队列的达托霉素浓度-时间数据进行了非参数群体药代动力学分析。进行了蒙特卡罗模拟,以比较标准达托霉素 6mg/kg/天剂量或 500mg 每日固定剂量在肥胖和非肥胖受试者中的最大浓度(C )、最小浓度(C )和曲线下面积(AUC)。用两种方案计算了超过达托霉素 C 目标(24.3mg/L 或更高)与肌酸磷酸激酶(CPK)升高相关的概率。

结果

在清除率、稳态分布容积或终末半衰期方面,肥胖和非肥胖 PK 模型之间没有观察到显著差异。达托霉素 6mg/kg/天导致肥胖受试者的 AUC、C 和 C 值相对于非肥胖个体高约 2 倍。相比之下,固定剂量(500mg/天)导致相对等剂量暴露。与 CPK 升高相关的 C 目标的模拟肥胖受试者的比例为 6mg/kg/天为 10.8%,500mg/天剂量为 2.0%。

结论

达托霉素的基于体重的维持剂量不太可能在病态肥胖受试者中产生生物等效暴露,并为评估跨成人体型的固定维持剂量以提高安全性提供了依据。

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