Versatile tissue‐injectable hydrogels capable of the extended hydrolytic release of bioactive protein therapeutics

Author:

Nealy Eric S.12ORCID,Reed Steven J.1ORCID,Adelmund Steven M.3ORCID,Badeau Barry A.3ORCID,Shadish Jared A.3ORCID,Girard Emily J.12ORCID,Brasel Kenneth12,Pakiam Fiona J.2ORCID,Mhyre Andrew J.12ORCID,Price Jason P.12,Sarkar Surojit145,Kalia Vandana15,DeForest Cole A.36789ORCID,Olson James M.1210ORCID

Affiliation:

1. Seattle Children's Research Institute Seattle Washington USA

2. Fred Hutch Cancer Center Seattle Washington USA

3. Department of Chemical Engineering University of Washington Seattle Washington USA

4. Department of Pathology University of Washington Seattle Washington USA

5. Department of Pediatrics University of Washington Seattle Washington USA

6. Department of Bioengineering University of Washington Seattle Washington USA

7. Department of Biochemistry University of Washington Seattle Washington USA

8. Department of Chemistry University of Washington Seattle Washington USA

9. Institute for Stem Cell and Regenerative Medicine, University of Washington Seattle Washington USA

10. Department of Pharmacology University of Washington Seattle Washington USA

Abstract

AbstractHydrogels are extensively employed in healthcare due to their adaptable structures, high water content, and biocompatibility, with FDA‐approved applications ranging from spinal cord regeneration to local therapeutic delivery. However, clinical hydrogels encounter challenges related to inconsistent therapeutic exposure, unmodifiable release windows, and difficulties in subsurface polymer insertion. Addressing these issues, we engineered injectable, biocompatible hydrogels as a local therapeutic depot, utilizing poly(ethylene glycol) (PEG)‐based hydrogels functionalized with bioorthogonal SPAAC handles for network polymerization and functionalization. Our hydrogel solutions polymerize in situ in a temperature‐sensitive manner, persist in tissue, and facilitate the delivery of bioactive therapeutics in subsurface locations. Demonstrating the efficacy of our approach, recombinant anti‐CD47 monoclonal antibodies, when incorporated into subsurface‐injected hydrogel solutions, exhibited cytotoxic activity against infiltrative high‐grade glioma xenografts in the rodent brain. To enhance the gel's versatility, recombinant protein cargos can undergo site‐specific modification with hydrolysable “azidoester” adapters, allowing for user‐defined release profiles from the hydrogel. Hydrogel‐generated gradients of murine CXCL10, linked to intratumorally injected hydrogel solutions via azidoester linkers, resulted in significant recruitment of CD8+ T‐cells and the attenuation of tumor growth in a “cold” syngeneic melanoma model. This study highlights a highly customizable, hydrogel‐based delivery system for local protein therapeutic administration to meet diverse clinical needs.

Funder

Israel National Road Safety Authority

National Science Foundation

National Institutes of Health

Alex's Lemonade Stand Foundation for Childhood Cancer

Howard Hughes Medical Institute

Publisher

Wiley

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