Issue 5, 2013

A glucose-responsive complex polymeric micelle enabling repeated on–off release and insulin protection

Abstract

We developed a glucose-responsive complex polymeric micelle (CPM) through the self-assembly of two types of diblock copolymers, poly(ethylene glycol)-b-poly(aspartic acid-co-aspartamidophenylboronic acid) (PEG-b-P(Asp-co-AspPBA)) and poly(N-isopropylacrylamide)-b-poly(aspartic acid-co-aspartamidophenylboronic acid) (PNIPAM-b-P(Asp-co-AspPBA)). By controlling the weight ratio between PNIPAM and PEG (WPNIPAM/WPEG = 6/4), the block copolymers form complex micelles with a novel core–shell–corona structure. By following this structure, the continuous PNIPAM shell collapsed on the glucose-responsive P(Asp-co-AspPBA) core. As a result, the CPM exhibits a reversible swelling in response to changes in the glucose concentration, enabling the repeated on–off release of insulin regulated by glucose level. Furthermore, the CPM could effectively protect the encapsulated insulin against protease degradation. Therefore, this glucose-responsive CPM provides a simple and powerful strategy to construct a self-regulated insulin delivery system for diabetes treatment.

Graphical abstract: A glucose-responsive complex polymeric micelle enabling repeated on–off release and insulin protection

Supplementary files

Article information

Article type
Paper
Submitted
22 Jul 2012
Accepted
29 Oct 2012
First published
11 Dec 2012

Soft Matter, 2013,9, 1636-1644

A glucose-responsive complex polymeric micelle enabling repeated on–off release and insulin protection

G. Liu, R. Ma, J. Ren, Z. Li, H. Zhang, Z. Zhang, Y. An and L. Shi, Soft Matter, 2013, 9, 1636 DOI: 10.1039/C2SM26690C

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