Evaluation of Aerosol Delivery of Nanosuspension for Pre-clinical Pulmonary Drug Delivery

被引:42
|
作者
Chiang, Po-Chang [1 ]
Alsup, Jason W. [1 ]
Lai, Yurong [1 ]
Hu, Yiding [1 ]
Heyde, Bruce R. [1 ]
Tung, David [1 ]
机构
[1] Pfizer Inc, Global Res & Dev, Pharmaceut Res & Dev, St Louis Labs, Chesterfield, MO USA
来源
NANOSCALE RESEARCH LETTERS | 2009年 / 4卷 / 03期
关键词
Lung inflammation; Intratracheal; Intranasal; Aerosol; Particle size; Pre-clinical; Impactor; Nano-suspension; PARTICLE-SIZE; DEPOSITION; LUNG; PHARMACOKINETICS; CORTICOSTEROIDS; FLUTICASONE; ABSORPTION;
D O I
10.1007/s11671-008-9234-1
中图分类号
TB3 [工程材料学];
学科分类号
0805 ; 080502 ;
摘要
Asthma and chronic obstructive pulmonary disease (COPD) are pulmonary diseases that are characterized by inflammatory cell infiltration, cytokine production, and airway hyper-reactivity. Most of the effector cells responsible for these pathologies reside in the lungs. One of the most direct ways to deliver drugs to the target cells is via the trachea. In a pre-clinical setting, this can be achieved via intratracheal (IT), intranasal (IN), or aerosol delivery in the desired animal model. In this study, we pioneered the aerosol delivery of a nanosuspension formulation in a rodent model. The efficiency of different dosing techniques and formulations to target the lungs were compared, and fluticasone was used as the model compound. For the aerosol particle size determination, a ten-stage cascade impactor was used. The mass median aerodynamic diameter (MMAD) was calculated based on the percent cumulative accumulation at each stage. Formulations with different particle size of fluticasone were made for evaluation. The compatibility of regular fluticasone suspension and nanosuspension for aerosol delivery was also investigated. The in vivo studies were conducted on mice with optimized setting. It was found that the aerosol delivery of fluticasone with nanosuspension was as efficient as intranasal (IN) dosing, and was able to achieve dose dependent lung deposition.
引用
收藏
页码:254 / 261
页数:8
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