Issue 9, 2016

Heparin-based hydrogels with tunable sulfation & degradation for anti-inflammatory small molecule delivery

Abstract

Sustained release of anti-inflammatory agents remains challenging for small molecule drugs due to their low molecular weight and hydrophobicity. Therefore, the goal of this study was to control the release of a small molecule anti-inflammatory agent, crystal violet (CV), from hydrogels fabricated with heparin, a highly sulfated glycosaminoglycan capable of binding positively-charged molecules such as CV. In this system, both electrostatic interactions between heparin and CV and hydrogel degradation were tuned simultaneously by varying the level of heparin sulfation and varying the amount of dithiothreitol within hydrogels, respectively. It was found that heparin sulfation significantly affected CV release, whereby more sulfated heparin hydrogels (Hep and Hep-N) released CV with near zero-order release kinetics (R-squared values between 0.96–0.99). Furthermore, CV was released more quickly from fast-degrading hydrogels than slow-degrading hydrogels, providing a method to tune total CV release between 5–15 days while maintaining linear release kinetics. In particular, N-desulfated heparin hydrogels exhibited efficient CV loading (∼90% of originally included CV), near zero-order CV release kinetics, and maintenance of CV bioactivity after release, making this hydrogel formulation a promising CV delivery vehicle for a wide range of inflammatory diseases.

Graphical abstract: Heparin-based hydrogels with tunable sulfation & degradation for anti-inflammatory small molecule delivery

Supplementary files

Article information

Article type
Paper
Submitted
08 Jul 2016
Accepted
15 Jul 2016
First published
22 Jul 2016

Biomater. Sci., 2016,4, 1371-1380

Heparin-based hydrogels with tunable sulfation & degradation for anti-inflammatory small molecule delivery

Y. Peng, L. E. Tellier and J. S. Temenoff, Biomater. Sci., 2016, 4, 1371 DOI: 10.1039/C6BM00455E

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