干粉吸入器
超临界流体
溶解
纳米医学
流化床
粒径
材料科学
活性成分
纳米颗粒
吸入器
微粉化
色谱法
喷雾干燥
药物输送
造粒
溶解试验
气溶胶化
化学工程
纳米技术
化学
吸入
药理学
医学
复合材料
有机化学
哮喘
生物制药分类系统
工程类
内科学
解剖
作者
Zhimin Ma,Xuejuan Zhang,Lu Ping,Zicheng Zhong,Xiubing Zhang,Xiaodong Zhuang,Guanlin Wang,Qiupin Guo,Shaofeng Zhan,Zhenwen Qiu,Ziyu Zhao,Qingguo Li,Dandong Luo
标识
DOI:10.1016/j.ijpharm.2023.123580
摘要
The supercritical antisolvent-fluidized bed coating process (SAS-FB) shows great potential as a technique to manufacture dry powder inhaler (DPI) that incorporate nanodrugs onto micronized matrix particles, capitalizing on the merits of both nanoparticle and pulmonary delivery. In this study, naringin (NAR), a pharmacologically active flavonoid with low solubility and in vivo degradation issues, was utilized as a model active pharmaceutical ingredient to construct nanomedicine-based DPI through SAS-FB. It is showed that processed NAR exhibited a near-spherical shape and an amorphous structure with an average size of around 130 nm. Notably, SAS-FB products prepared with different fluidized matrices resulted in varying deposition patterns, particularly when mixed with a coarse lactose to enhance the fine particle fraction (FPF) of the formulations. The FPF was positively associated with specific surface area of the SAS-FB products, while the specific surface area was directly related to surface roughness and particle size. In vitro dissolution studies using simulated lung fluid revealed that the NAR nanoparticles coated on the products were released immediately upon contact with solution, with a cumulative dissolution exceeding 90% within the first minute. Importantly, compared to oral raw NAR, the optimized DPI formulation demonstrated superior in vivo plasmatic and pulmonary AUC0→∞ by 51.33-fold and 104.07-fold respectively in a Sprague-Dawley rat model. Overall, SAS- FB technology provides a practical approach to produce nanomedicine DPI product that combine the benefits of nanoparticles with the aerodynamics properties of inhaled microparticles.
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