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基于 mPEG-PLA 的载药纳米粒的研制与评价:体外与体内研究。

Development and evaluation of nanoparticles based on mPEG-PLA for controlled delivery of vinpocetine: in vitro and in vivo studies.

机构信息

a Department of Pharmaceutical , 85 Hospital of People's Liberation Army , Shanghai , China.

出版信息

Artif Cells Nanomed Biotechnol. 2017 Feb;45(1):157-162. doi: 10.3109/21691401.2016.1138492. Epub 2016 Feb 2.

Abstract

The aim of present study was to develop VIN-loaded mPEG-PLA nanoparticle systems. The VIN mPEG-PLA nanoparticles were prepared using an emulsion solvent evaporation method, and studied their particle size, morphology, encapsulation efficiency and drug-loading coefficient. Moreover, the nanoparticles were evaluated on the drug release behaviors in vitro and bioavailability in vivo. The results show that the spherical nanoparticles obtained were negatively charged with a zeta potential of about -23.4 mV and characterized ∼110 nm with a narrow size distribution. The encapsulation efficiency and drug loading of prepared NPs were 76.4 ± 6.3 and 9.2 ± 2.2% (n=5), respectively. The in vitro release showed that the percent of accumulated dissolution of VIN NPs in phosphate-buffered saline 6.8 over 24 h was <80%, which was almost 100% of VIN in commercial injections. The in vivo study indicated that systemic absorption of VIN was significantly enhanced by incorporating into mPEG-PLA NPs compared with VIN injection (2.87-fold in AUC). The results suggested that the form of VIN in mPEG-PLA NPs could enter the body circulation to perform sustained release in vitro and in vivo.

摘要

本研究旨在开发载长春西汀(VIN)的 mPEG-PLA 纳米粒系统。采用乳化溶剂蒸发法制备 VIN-mPEG-PLA 纳米粒,并研究其粒径、形态、包封率和载药量。此外,还评估了纳米粒的体外释放行为和体内生物利用度。结果表明,得到的球形纳米粒带负电荷,zeta 电位约为-23.4 mV,粒径分布较窄,约为 110nm。制备的 NPs 的包封率和载药量分别为 76.4±6.3%和 9.2±2.2%(n=5)。体外释放结果显示,VIN NPs 在磷酸盐缓冲盐水(PBS)中 24 h 的累积溶出度<80%,几乎是市售注射液中 VIN 的 100%。体内研究表明,与 VIN 注射液相比,将 VIN 包载于 mPEG-PLA NPs 中可显著提高 VIN 的全身吸收(AUC 增加 2.87 倍)。结果表明,mPEG-PLA NPs 中的 VIN 形式可进入体循环,在体外和体内实现持续释放。

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