4.7 Article

Initial Steps towards Spatiotemporal Signaling through Biomaterials Using Click-to-Release Chemistry

Journal

PHARMACEUTICS
Volume 14, Issue 10, Pages -

Publisher

MDPI
DOI: 10.3390/pharmaceutics14101991

Keywords

click chemistry; bio-orthogonal chemistry; trans-cyclooctene; tetrazine; controlled release; collagen scaffolds; wound healing; regenerative medicine

Funding

  1. Radboudumc RIMLS Young Investigator Grant

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In this study, the feasibility of using click-to-release chemistry to develop pro-regenerative biomaterials was demonstrated. The release of anti-fibrotics from tunable biomaterials was achieved, thus promoting regeneration in wound healing.
The process of wound healing is a tightly controlled cascade of events, where severe skin wounds are resolved via scar tissue. This fibrotic response may be diminished by applying anti-fibrotic factors to the wound, thereby stimulating regeneration over scarring. The development of tunable biomaterials that enable spatiotemporal control over the release of anti-fibrotics would greatly benefit wound healing. Herein, harnessing the power of click-to-release chemistry for regenerative medicine, we demonstrate the feasibility of such an approach. For this purpose, one side of a bis-N-hydroxysuccinimide-trans-cyclooctene (TCO) linker was functionalized with human epidermal growth factor (hEGF), an important regulator during wound healing, whereas on the other side a carrier protein was conjugated-either type I collagen scaffolds or bovine serum albumin (BSA). Mass spectrometry demonstrated the coupling of hEGF-TCO and indicated a release following exposure to dimethyl-tetrazine. Type I collagen scaffolds could be functionalized with the hEGF-TCO complex as demonstrated by immunofluorescence staining and Western blotting. The hEGF-TCO complex was also successfully ligated to BSA and the partial release of hEGF upon dimethyl-tetrazine exposure was observed through Western blotting. This work establishes the potential of click-to-release chemistry for the development of pro-regenerative biomaterials.

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