PLGA公司
乙二醇
体内
聚乙二醇
纳米颗粒
粘液
材料科学
PEG比率
生物物理学
药物输送
黏膜黏附
离体
化学
毒品携带者
纳米技术
体外
化学工程
纳米载体
有机化学
生物化学
财务
工程类
生态学
经济
生物
生物技术
作者
Qingguo Xu,Laura M. Ensign,Nicholas J. Boylan,Arne Schön,Xiaoqun Gong,Jeh‐Chang Yang,Nicholas W. Lamb,Shutian Cai,Tao Yu,Ernesto Freire,Justin Hanes
出处
期刊:ACS Nano
[American Chemical Society]
日期:2015-08-31
卷期号:9 (9): 9217-9227
被引量:438
标识
DOI:10.1021/acsnano.5b03876
摘要
Achieving sustained drug delivery to mucosal surfaces is a major challenge due to the presence of the protective mucus layer that serves to trap and rapidly remove foreign particulates. Nanoparticles engineered to rapidly penetrate mucosal barriers (mucus-penetrating particles, “MPP”) have shown promise for improving drug distribution, retention and efficacy at mucosal surfaces. MPP are densely coated with polyethylene glycol (PEG), which shields the nanoparticle core from adhesive interactions with mucus. However, the PEG density required to impart the “stealth” properties to nanoparticles in mucus, and thus, uniform distribution in vivo, is still unknown. We prepared biodegradable poly(lactic-co-glycolic acid) (PLGA) nanoparticles with a range of PEG surface densities by blending various ratios of a diblock copolymer of PLGA and 5 kDa poly(ethylene glycol) (PLGA–PEG5k) with PLGA. We then evaluated the impact of PEG surface density, measured using an 1H NMR method, on mucin binding in vitro, nanoparticle transport in freshly obtained human cervicovaginal mucus (CVM) ex vivo, and nanoparticle distribution in the mouse cervicovaginal tract in vivo. We found that at least 5% PEG was required to effectively shield the nanoparticle core from interacting with mucus components in vitro and ex vivo, thus leading to enhanced nanoparticle distribution throughout the mouse vagina in vivo. We then demonstrated that biodegradable MPP could be formulated from blends of PLGA and PLGA–PEG polymers of various molecular weights, and that these MPP provide tunable drug loading and drug release rates and durations. Overall, we describe a methodology for rationally designing biodegradable, drug-loaded MPP for more uniform delivery to the vagina.
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