β-Lactoglobulin stabilized lipid nanoparticles enhance oral absorption of insulin by slowing down lipolysis

被引:0
|
作者
Lu Li [1 ]
Suticha Chunta [2 ]
Xianzi Zheng [1 ]
Haisheng He [1 ]
Wei Wu [1 ,3 ,4 ]
Yi Lu [1 ,3 ,4 ]
机构
[1] School of Pharmacy & Key Laboratory of Smart Drug Delivery of MOE, Fudan University
[2] Department of Clinical Chemistry, Faculty of Medical Technology, Prince of Songkla University
[3] Shanghai Skin Disease Hospital, Tongji University School of Medicine
[4] Fudan Zhangjiang Institute
基金
中国国家自然科学基金;
关键词
D O I
暂无
中图分类号
R943 [制剂学]; TB383.1 [];
学科分类号
070205 ; 080501 ; 100602 ; 100702 ; 1406 ;
摘要
Lipid-based nanocarriers have staged a remarkable comeback in the oral delivery of proteins and peptides, but delivery efficiency is compromised by lipolysis. β-Lactoglobulin(β-lg) stabilized lipid nanoparticles, including nanoemulsions(NE@β-lg) and nanocapsules(NC@β-lg), were developed to enhance the oral absorption of insulin by slowing down lipolysis due to the protection from β-lg. Cremophor EL stabilized nanoemulsions(NE@Cre-EL) were prepared and set as a control. The lipid nanoparticles produced mild and sustained hypoglycemic effects, amounting to oral bioavailability of 3.0% ± 0.3%, 7.0% ± 1.1%, and7.7% ± 0.8% for NE@Cre-EL, NE@β-lg, and NC@β-lg, respectively. Aggregation-caused quenching(ACQ)probes enabled the identification of intact nanoparticles, which were used to investigate the in vivo and intracellular fates of the lipid nanoparticles. In vitro digestion/lipolysis and ex vivo imaging confirmed delayed lipolysis from β-lg stabilized lipid nanoparticles. NC@β-lg was more resistant to intestinal lipolysis than NE@β-lg due to the Ca2+-induced crosslinking. Live imaging revealed the transepithelial transport of intact nanoparticles and their accumulation in the liver. Cellular studies confirmed the uptake of intact nanoparticles. Slowing down lipolysis via food proteins represents a good strategy to enhance the oral absorption of lipid nanoparticles and thus co-formulated biomacromolecules.
引用
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页码:313 / 317
页数:5
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