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Folic acid-modified reverse micelle-lipid nanocapsules overcome intestinal barriers and improve the oral delivery of peptides.
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- Author(s): He, Jibiao1 (AUTHOR); Ding, Ruihuan1 (AUTHOR); Tao, Yuping1 (AUTHOR); Zhao, Zhenyu2 (AUTHOR); Yuan, Ranran2 (AUTHOR); Zhang, Houqian2 (AUTHOR); Wang, Aiping1 (AUTHOR); Sun, Kaoxiang1 (AUTHOR); Li, Youxin1,3 (AUTHOR); Shi, Yanan2 (AUTHOR)
- Source:
Drug Delivery. Dec2023, Vol. 30 Issue 1, p1-11. 11p.
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- Additional Information
- Abstract:
The oral absorption of exenatide, a type 2 diabetes medication, can be increased by employing lipid nanocapsules (LNC). To increase mucus permeability and exenatide intestinal absorption, reverse micelle lipid nanocapsules (RM-LNC) were prepared and their surface was modified with DSPE-PEG-FA. The RM-LNC with surface modification of DSPE-PEG-FA (FA-RM-LNC) were able to target enterocytes and reduce mucus aggregation in the intestine. Furthermore, in vitro absorption at different intestinal sites and flip-flop intestinal loop experiments revealed that LNCs with surface modification significantly increased their absorption efficiency in the small intestine. FA-RM-LNC delivers more drugs into Caco-2 cells via caveolin-, macrophagocytosis-, and lipid raft-mediated endocytosis. Additionally, the enhanced transport capacity of FA-RM-LNC was observed in a study of monolayer transport in Caco-2 cells. The oral administration of exenatide FA-RM-LNC resulted in a prolonged duration of hypoglycemia in diabetic mice and a relative bioavailability (BR) of up to 7.5% in rats. In conclusion, FA-RM-LNC can target enterocytes and has promising potential as a nanocarrier for the oral delivery of peptides. [ABSTRACT FROM AUTHOR]
- Abstract:
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