| Literature DB >> 30601014 |
Yina Song1, Yanan Shi2, Liping Zhang1, Haiyan Hu1, Chunyan Zhang1, Miaomiao Yin1, Liuxiang Chu1, Xiuju Yan1, Mingyu Zhao1, Xuemei Zhang3, Hongjie Mu1, Kaoxiang Sun1,3.
Abstract
The oral absorption of exenatide, a drug for type 2 diabetes treatment, can be improved by using nanoparticles (NPs) for its delivery. To improve the mucus penetration and intestinal absorption of exenatide, we designed a block copolymer, CSKSSDYQC-dextran-poly(lactic-co-glycolic acid) (CSK-DEX-PLGA), and used it for the preparation of exenatide-loaded NPs. The functionalized exenatide-loaded NPs composed of CSK-DEX-PLGA were able to target intestinal epithelial cells and reduce the mucus-blocking effect of the intestine. Moreover, the CSK modification of DEX-PLGA was found to significantly promote the absorption efficiency of NPs in the small intestine based on in vitro ligation of the intestinal rings and an examination of different intestinal absorption sites. Compared to DEX-PLGA-NPs (DPs), the absorption of CSK-DEX-PLGA-NPs (CDPs) was increased in the villi, allowing the drug to act on gobletlike Caco-2 cells through clathrin-, caveolin-, and gap-mediated endocytosis. Furthermore, the enhanced transport ability of CDPs was observed in a study on Caco-2/HT-29-MTX cocultured cells. CDPs exhibited a prolonged hypoglycemic response with a relative bioavailability of 9.2% in diabetic rats after oral administration. In conclusion, CDPs can target small intestinal goblet cells and have a beneficial effect on the oral administration of macromolecular peptides as a nanometer-sized carrier.Entities:
Keywords: intestinal absorption; mucus penetration; oral delivery; targeted nanoparticle
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Year: 2019 PMID: 30601014 DOI: 10.1021/acs.molpharmaceut.8b00809
Source DB: PubMed Journal: Mol Pharm ISSN: 1543-8384 Impact factor: 4.939