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基于身高的妥布霉素初始剂量列线图在成人囊性纤维化肺部感染加重治疗中的开发和评估。

Development and Evaluation of a Height-Based Tobramycin Initial Dosing Nomogram for the Treatment of Adult Cystic Fibrosis Pulmonary Exacerbations.

机构信息

Faculté de pharmacie, Université de Montréal, Montreal, Canada.

Laboratoire de suivi thérapeutique pharmacologique et pharmacocinétique, Faculté de pharmacie, Université de Montréal, Montreal, Canada.

出版信息

Ther Drug Monit. 2023 Apr 1;45(2):259-264. doi: 10.1097/FTD.0000000000001053.

Abstract

Tobramycin is widely used to treat pulmonary exacerbations of cystic fibrosis. Height has been previously found to be significantly more predictive of tobramycin pharmacokinetics than body weight. This study aimed to develop a height-based initial dosing nomogram and evaluate its performance in peak concentration (Cmax) precision relative to standard and fixed dosing. Monte Carlo simulations were performed to develop a nomogram representing the doses required to reach Cmax targets at different heights. Cmax data observed at 2 clinical centers [McGill University Health Centre (MUHC) and Institut universitaire de cardiologie et pneumologie de Québec (IUCPQ-UL)] were compared with population-predicted Cmax using the doses derived from the nomogram alongside a fixed dose. Height-based dosing resulted in significantly less variable-predicted Cmax values [coefficient of variation (CV) MUHC = 15.7% and IUCPQ-UL = 10.8%] than the Cmax values observed in clinical practice (CV MUHC = 30.0% and CV IUCPQ-UL = 26.9%) and predicted Cmax values obtained from a fixed dose (CV MUHC = 21.2% and CV IUCPQ-UL = 16.3%). An initial dosing nomogram was developed to help reduce pharmacokinetic variability in the observed Cmax. More precise dosing would allow for better clinical outcomes in adult patients with cystic fibrosis.

摘要

妥布霉素被广泛用于治疗囊性纤维化的肺部恶化。先前发现身高对妥布霉素药代动力学的预测性明显高于体重。本研究旨在开发一种基于身高的初始剂量列线图,并评估其在峰值浓度(Cmax)精度方面相对于标准和固定剂量的性能。通过蒙特卡罗模拟开发了一个列线图,代表在不同高度达到 Cmax 目标所需的剂量。使用从列线图得出的剂量以及固定剂量,比较了在 2 个临床中心(麦吉尔大学健康中心(MUHC)和魁北克心脏研究所和肺病学研究所(IUCPQ-UL))观察到的 Cmax 数据与人群预测的 Cmax。基于身高的剂量导致预测的 Cmax 值的变异性显著降低[MUHC 的变异系数(CV)= 15.7%和 IUCPQ-UL = 10.8%],低于临床实践中观察到的 Cmax 值(MUHC 的 CV = 30.0%和 CV IUCPQ-UL = 26.9%)和从固定剂量获得的预测 Cmax 值(MUHC 的 CV = 21.2%和 CV IUCPQ-UL = 16.3%)。开发了一个初始剂量列线图,以帮助降低观察到的 Cmax 的药代动力学变异性。更精确的剂量可以为囊性纤维化的成年患者带来更好的临床结果。

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