LI Wei-wei, WANG Yi-ting, SHEN Mei, et al. Preparation of mPEG-PCL Polymersomes and Release Investigation of Insulin-loaded mPEG-PCL Polymersomes[J]. Chinese journal of experimental traditional medical formulae, 2014, 20(23): 15-21.
DOI:
LI Wei-wei, WANG Yi-ting, SHEN Mei, et al. Preparation of mPEG-PCL Polymersomes and Release Investigation of Insulin-loaded mPEG-PCL Polymersomes[J]. Chinese journal of experimental traditional medical formulae, 2014, 20(23): 15-21. DOI: 10.13422/j.cnki.syfjx.2014230015.
Preparation of mPEG-PCL Polymersomes and Release Investigation of Insulin-loaded mPEG-PCL Polymersomes
Objective: To prepare mPEG-PCL copolymer and polymersomes
then investigate in vitro release of INS-mPEG114-PCL152 polymersomes. Method: mPEG-PCL block copolymer was synthesized by ring-opening polymerization method
chemical structure of these polymers were characterized by FT-IR and 1H-NMR.Polymersomes were prepared by film hydration method
particle size and apparent morphology were examined by dynamic light scattering and transmission electron microscope
respectively;critical aggregation concentration(CAC) was detected by fluorescence techniques with pyrene as a probe.Encapsulation efficiency
drug loading and in vitro release characteristic of INS-mPEG114-PCL152 polymersomes were determined by Bradford method. Result: Average particle sizes of blank polymersomes were about 200 nm
CAC were all low value.These prepared INS-mPEG114-PCL152 with 20% drug-copolymer ratio had maximize utilizaiton ratio
average encapsulation efficiency (62.80±2.14)% as well as drug loading (11.10±0.34)%.In vitro cumulative release of INS-mPEG114-PCL152 polymersomes in 48 h was about 55.05%
with relatively significant burst release at initial 2 h about 19.28%. Conclusion: These polymersomes have uniform particle size with a great anti-dilution capability.INS-mPEG114-PCL152 polymersomes show a significant burst release at initial stage and then a good sustained-release property with dissociation of surface model drug.
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