Department of Pharmacy, Northwestern Memorial Hospital, Chicago, Illinois.
Department of Pharmacy Practice, Midwestern University Chicago College of Pharmacy, Downers Grove, Illinois.
Pharmacotherapy. 2020 Jun;40(6):584-591. doi: 10.1002/phar.2399. Epub 2020 May 5.
Systemic aminoglycosides remain a cornerstone of treatment for cystic fibrosis (CF) pulmonary exacerbations (PEx); however, the impact of aminoglycoside pharmacokinetics (PK) on outcomes is not well defined in adult CF patients. Our objective was to assess the impact of increasing PK exposures on the clinical outcomes of PEx treatment in adult CF patients receiving high-dose and standard-dose extended-interval aminoglycosides.
We conducted a retrospective study of adult CF patients treated with an intravenous aminoglycoside for a PEx. Serum amikacin, gentamicin, and tobramycin levels and forced expiratory volume over 1 second (FEV ) data were used to evaluate exposure-response relationships. PK parameters were estimated using a Bayesian approach to obtain area under the curve (AUC) , maximum concentration (C ), and minimum concentration (Cmin ) estimates. The primary efficacy end point was a 90% recovery of baseline FEV by 30 days posttreatment. Toxicity included signs or symptoms of ototoxicity, vestibular toxicity, or renal toxicity. Multivariate linear mixed-effects models of FEV were used for exposure-response analysis.
The study included 51 patients who contributed 188 FEV observations. There were 3.0 ± 1.7 (mean ± SD) aminoglycoside concentrations per patient. The mean AUC , C , and C across all agents and patients were 156 ± 96 mg*hr/L, 29.9 ± 12.7 mg/L, and 0.35 ± 0.66 mg/L, respectively. A total of 42 amikacin-, gentamicin-, or tobramycin-treated patients contributed to the efficacy analysis, of whom 85.7% experienced recovery posttreatment. Of the 51 included patients, 6 (11.8%) experienced seven toxicity events. In exploratory exposure-response analyses, neither AUC nor C was associated with FEV values after adjusting for clinical covariates and baseline FEV .
Increasing aminoglycoside AUC and C were not associated with FEV during PEx treatment. Although individualizing aminoglycoside dosing in adult CF patients is necessary to minimize toxicity risk, more work is needed to define optimally safe and effective dosing strategies for this population.
全身性氨基糖苷类药物仍然是囊性纤维化(CF)肺部恶化(PEx)治疗的基石;然而,在成年 CF 患者中,氨基糖苷类药物药代动力学(PK)对结局的影响尚不清楚。我们的目的是评估增加 PK 暴露对接受高剂量和标准剂量延长间隔氨基糖苷类药物治疗的成年 CF 患者 PEx 治疗临床结局的影响。
我们对接受静脉内氨基糖苷类药物治疗 PEx 的成年 CF 患者进行了回顾性研究。使用血清阿米卡星、庆大霉素和妥布霉素水平和 1 秒用力呼气量(FEV )数据来评估暴露-反应关系。使用贝叶斯方法估计 PK 参数,以获得 AUC 、 C 和 Cmin 的估计值。主要疗效终点是治疗后 30 天内 FEV 恢复基线的 90%。毒性包括耳毒性、前庭毒性或肾毒性的体征或症状。FEV 的多变量线性混合效应模型用于暴露-反应分析。
该研究纳入了 51 名患者,共提供了 188 次 FEV 观察结果。每位患者有 3.0±1.7 个(平均值±标准差)氨基糖苷类药物浓度。所有药物和患者的 AUC 、 C 和 C 平均值分别为 156±96mg*hr/L、29.9±12.7mg/L 和 0.35±0.66mg/L。共有 42 名接受阿米卡星、庆大霉素或妥布霉素治疗的患者参与了疗效分析,其中 85.7%在治疗后恢复。在 51 名纳入患者中,有 6 名(11.8%)发生了 7 起毒性事件。在探索性暴露-反应分析中,在调整临床协变量和基线 FEV 后,AUC 或 C 均与 FEV 值无关。
在 PEx 治疗期间,增加氨基糖苷类药物的 AUC 和 C 与 FEV 无关。虽然在成年 CF 患者中个体化氨基糖苷类药物剂量以最小化毒性风险是必要的,但仍需要更多的工作来为该人群定义最佳安全有效的给药策略。
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