Issue 9, 2012

PEG-urokinase nanogels with enhanced stability and controllable bioactivity

Abstract

Protein nanogels were synthesized via a one-step reaction procedure by crosslinking urokinase with benzaldehyde bifunctionalized poly(ethylene glycol). The crosslinked architecture significantly enhances the stability of urokinase against enzyme degradation in comparison with the core–shell structural PEGylated proteins. Meanwhile, bioactivity of the urokinase incorporated in the nanogels can be adjusted by varying the chain length of the corsslinking polymer. With a shorter crosslinker the bioactivity of the uPA nanogels is seriously restricted under physiological conditions. However, the restricted bioactivity can be completely launched by either enlarging the mesh size of the nanogel by using longer crosslinkers, or treating the nanogels in endosomal conditions to dissociate the nanogel structure due to the reversible conjugation chemistry.

Graphical abstract: PEG-urokinase nanogels with enhanced stability and controllable bioactivity

Supplementary files

Article information

Article type
Paper
Submitted
31 Oct 2011
Accepted
05 Dec 2011
First published
23 Jan 2012

Soft Matter, 2012,8, 2644-2650

PEG-urokinase nanogels with enhanced stability and controllable bioactivity

H. Tan, H. Jin, H. Mei, L. Zhu, W. Wei, Q. Wang, F. Liang, C. Zhang, J. Li, X. Qu, D. Shangguan, Y. Huang and Z. Yang, Soft Matter, 2012, 8, 2644 DOI: 10.1039/C2SM07072C

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