Title of article :
Sustained-release study on Exenatide loaded into mesoporous silica nanoparticles: in vitro characterization and in vivo evaluation
Author/Authors :
Chen, Cuiwei Department of Pharmaceutics - Zhejiang Chinese Medical University - Hangzhou 311042 - China , Zheng, Hongyue Libraries of Zhejiang Chinese Medical University Zhejiang Chinese Medical University - Hangzhou 310053 - China , Xu, Junjun Department of Pharmacy - The Second Affiliated Hospital - School of Medicine - Zhejiang University - Hangzhou 310052 - China , Shi, Xiaowei Department of Pharmaceutics - Zhejiang Chinese Medical University - Hangzhou 311042 - China , Li, Fanzhu Department of Pharmaceutics - Zhejiang Chinese Medical University - Hangzhou 311042 - China , Wang, Xuanshen Department of Pharmacy - The Second Hospital of Dalian Medical University - Dalian 116027 - China
Abstract :
Background: Exenatide (EXT), the first glucagon-like peptide-1 receptor agonist, has been approved as an adjunctive therapy for patients with type 2 diabetes. Due to EXT’s short half-life, EXT must be administrated by
continuous subcutaneous (s.c.) injection twice daily. In previous studies, many studies on EXT loaded into polymer
materials carriers for sustained release had been reported. However, these carriers have some defects, such as
hydrophobicity, low surface energy, low mechanical strength, and poor chemical stability. Therefore, this study
aims to develop a novel drug delivery system, which is EXT loaded into well-ordered hexagonal mesoporous
silica structures (EXT-SBA-15), to control the sustainability of EXT.
Methods: SBA-15 was prepared by hydrothermal method with uniform size. Morphology of SBA-15 was employed
by transmission electron microscopy. The pore size of SBA-15 was characterized by N2 adsorption–desorption
isotherms. The in vitro drug release behavior and pharmacokinetics of EXT-SBA-15 were investigated. Furthermore,
the blood glucose levels of diabetic mice were monitored after subcutaneous injection of EXT-Sol and EXT-SBA-15
to evaluate further the stable hypoglycemic effect of EXT-SBA-15.
Results: EXT-SBA-15 showed a higher drug loading efficiency (15.2 ± 2.0%) and sustained-release features in vitro.
In addition, pharmacokinetic studies revealed that the EXT-SBA-15 treatment group extended the half-life t1/2(β) to
14.53 ± 0.70 h compared with that of the EXT solution (EXT-Sol) treatment group (0.60 ± 0.08 h) in vivo. Results of
the pharmacodynamics study show that the EXT-SBA-15 treatment group had inhibited blood glucose levels below
20 mmol/L for 25 days, and the lowest blood glucose level was 13 mmol/L on the 10th day.
Conclusions: This study demonstrates that the EXT-SBA-15 delivery system can control the sustainability of EXT and contribute to improve EXT clinical use.
Keywords :
Exenatide , Type 2 diabetic , Mesoporous silica nanoparticles , Sustained release , Pharmacokinetics/ Pharmacodynamics
Journal title :
Daru:Journal of Pharmaceutical Sciences
