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Oral delivery of an anti-diabetic peptide drug via conjugation and complexation with low molecular weight chitosan

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Abstract
Despite the therapeutic potential of exendin-4 as a glucagon-like peptide-1 (GLP-1) mimetic for the treatment of type 2 diabetes, its utility has so far been limited because of the low level of patient compliance due to the requirement for frequent injections. In this study, an orally available exendin-4 was produced by conjugating it to low molecular weight chitosan (LMWC). Conjugation between the LMWC and cysteinylated exendin-4 was carried out using a cleavable linker system in order to maximize the availability of the active peptide. The LMWC-exendin-4 conjugate formed a nanoparticle structure with a mean particle size of 101 +/- 41 nm through complexation between the positively charged LMWC backbone and the negatively charged exendin-4 of individual conjugate molecules. The biological activity of the LMWC-exendin-4 conjugatewas evaluated in an INS-1 cell line. The LMWC-exendin-4 conjugate stimulated insulin secretion in a dose dependent manner as similar as that of native exendin-4. From the pharmacokinetic study after oral administration of the conjugate, a C-max value of 344 pg/mL and a T-max of 6 h were observed, and the bioavailability, relative to the subcutaneous counterpart, was found to be 6.4%. Furthermore, the absorbed exendin-4 demonstrated a significantly enhanced hypoglycemic effect. These results suggest that the LMWC-exendin-4 conjugate could be used as a potential oral antidiabetic agent for the treatment of type 2 diabetes. (C) 2013 Elsevier B. V. All rights reserved.
Author(s)
Ahn, SukyungLee, In-HyunLee, EunhyeKim, HyungjunKim, Yong-ChulJon, Sangyong
Issued Date
2013-09
Type
Article
DOI
10.1016/j.jconrel.2013.05.031
URI
https://scholar.gist.ac.kr/handle/local/15441
Publisher
Elsevier BV
Citation
Journal of Controlled Release, v.170, no.2, pp.226 - 232
ISSN
0168-3659
Appears in Collections:
Department of Life Sciences > 1. Journal Articles
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