| Literature DB >> 29055774 |
Weiwei Fan1, Dengning Xia2, Quanlei Zhu2, Xiuying Li3, Shufang He1, Chunliu Zhu2, Shiyan Guo2, Lars Hovgaard4, Mingshi Yang5, Yong Gan6.
Abstract
Oral absorption of protein/peptide-loaded nanoparticles is often limited by multiple barriers of the intestinal epithelium. In addition to mucus translocation and apical endocytosis, highly efficient transepithelial absorption of nanoparticles requires successful intracellular trafficking, especially to avoid lysosomal degradation, and basolateral release. Here, the functional material, deoxycholic acid-conjugated chitosan, is synthesized and loaded with the model protein drug insulin into deoxycholic acid-modified nanoparticles (DNPs). The DNPs designed in this study are demonstrated to overcome multiple barriers of the intestinal epithelium by exploiting the bile acid pathway. In Caco-2 cell monolayers, DNPs are internalized via apical sodium-dependent bile acid transporter (ASBT)-mediated endocytosis. Interestingly, insulin degradation in the epithelium is significantly prevented due to endolysosomal escape of DNPs. Additionally, DNPs can interact with a cytosolic ileal bile acid-binding protein that facilitates the intracellular trafficking and basolateral release of insulin. In rats, intravital two-photon microscopy also reveals that the transport of DNPs into the intestinal villi is mediated by ASBT. Further pharmacokinetic studies disclose an oral bioavailability of 15.9% in type I diabetic rats after loading freeze-dried DNPs into enteric-coated capsules. Thus, deoxycholic acid-modified chitosan nanoparticles can overcome multiple barriers of the intestinal epithelium for oral delivery of insulin.Entities:
Keywords: Bile acid pathway; Endolysosomal escape; Functional nanoparticles; Insulin; Intestinal epithelium; Oral delivery
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Year: 2017 PMID: 29055774 DOI: 10.1016/j.biomaterials.2017.10.022
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479