应用群体药代动力学特征描述丙酸氟替卡松干粉吸入剂在人体中的肺部中央和周边沉积。
Central and peripheral lung deposition of fluticasone propionate dry powder inhaler formulations in humans characterized by population pharmacokinetics.
机构信息
Department of Pharmaceutics, College of Pharmacy, University of Florida, Box 100494, Gainesville, FL, 32610, USA.
Department of Pharmacotherapy and Translational Research, College of Pharmacy, University of Florida, 6550 Sanger Road, Orlando, FL, 32827, USA.
出版信息
Pharm Res. 2023 May;40(5):1177-1191. doi: 10.1007/s11095-023-03472-6. Epub 2023 Apr 20.
This study aimed to gain an in-depth understanding of the pulmonary fate of three experimental fluticasone propionate (FP) dry powder inhaler formulations which differed in mass median aerodynamic diameters (MMAD; A-4.5 µm, B-3.8 µm and C-3.7 µm; total single dose: 500 µg). Systemic disposition parameter estimates were obtained from published pharmacokinetic data after intravenous dosing to improve robustness. A biphasic pulmonary absorption model, with mucociliary clearance from the slower absorption compartment, and three systemic disposition compartments was most suitable. Rapid absorption, presumably from peripheral lung, had half-lives of 6.9 to 14.6 min. The peripherally deposited dose (12.6 µg) was significantly smaller for formulation A-4.5 µm than for the other formulations (38.7 and 39.3 µg for B-3.8 µm and C-3.7 µm). The slow absorption half-lives ranged from 6.86 to 9.13 h and were presumably associated with more central lung regions, where mucociliary clearance removed approximately half of the centrally deposited dose. Simulation-estimation studies showed that a biphasic absorption model could be reliably identified and that parameter estimates were unbiased and reasonably precise. Bioequivalence assessment of population pharmacokinetics derived central and peripheral lung doses suggested that formulation A-4.5 µm lacked bioequivalence compared to the other formulations both for central and peripheral doses. In contrast, the other fomulations were bioequivalent. Overall, population pharmacokinetics holds promise to provide important insights into the pulmonary fate of inhalation drugs, which are not available from non-compartmental analysis. This supports the assessment of the pulmonary bioequivalence of fluticasone propionate inhaled formulations through pharmacokinetic approaches, and may be helpful for discussions on evaluating alternatives to clinical endpoint studies.
本研究旨在深入了解三种实验性丙酸氟替卡松干粉吸入剂制剂的肺部命运,这三种制剂的质量中值空气动力学直径(MMAD;A-4.5μm、B-3.8μm 和 C-3.7μm;总单剂量:500μg)不同。通过静脉注射给药获得的已发表药代动力学数据来估计系统处置参数,以提高稳健性。具有从较慢吸收隔室清除的黏液纤毛清除作用的两相肺部吸收模型和三个系统处置隔室最适合。快速吸收,推测来自外周肺,半衰期为 6.9 至 14.6 分钟。对于 A-4.5μm 制剂,外周沉积剂量(12.6μg)明显小于其他制剂(B-3.8μm 和 C-3.7μm 制剂分别为 38.7μg 和 39.3μg)。慢吸收半衰期范围为 6.86 至 9.13 小时,推测与更中央的肺区域有关,其中黏液纤毛清除作用去除了大约一半的中央沉积剂量。模拟估计研究表明,两相吸收模型可以可靠地识别,并且参数估计无偏且相当精确。基于群体药代动力学的中央和外周肺剂量的生物等效性评估表明,与其他两种制剂相比,A-4.5μm 制剂在中央和外周剂量方面均缺乏生物等效性。相比之下,其他制剂是生物等效的。总体而言,群体药代动力学有望为吸入药物的肺部命运提供重要的见解,这些见解无法从非房室分析中获得。这支持通过药代动力学方法评估吸入丙酸氟替卡松制剂的肺部生物等效性,并且可能有助于讨论评估替代临床终点研究的方法。
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