Oxidation-responsive, settable bone substitute composites for regenerating critically-sized bone defects

Abstract

Critically-sized bone defects that cannot spontaneously heal on their own remain a significant problem in the clinic. Synthetic polymeric implants are promising therapies for improving bone healing as they are highly tunable and avoid the potential complications associated with autologous bone grafts. However, biostable implants such as poly(methyl methacrylate (PMMA) suffer from numerous shortcomings including negligible biodegradability and limited osseointegration with bone. Hydrolytically-degradable polymeric implants such as poly(caprolactone) (PCL) or poly(lactic-co-glycolic acid) (PLGA) have shown promise facilitating bone growth before being resorbed, but matching the degradation rate of these polyesters with the rate of bone regeneration continues to be an engineering challenge. To address these limitations with current synthetic bone implant materials, cell-degradable polymer / hydroxyapatite composites were developed as in situ-curing bone substitutes. The polymeric component was formulated from a thioketal (TK) dithiol linker and a tri-functional epoxy to enable rapid crosslinking upon deployment. To enable biologically-responsive implant resorption, the TK unit is specifically cleaved by cell-produced reactive oxygen species (ROS). TK bone substitutes possessed tunable curing and mechanical properties, were selectively degraded in dose-dependent concentrations of ROS, were non-cytotoxic, and demonstrated significantly greater bone regeneration capacity than PMMA in a critically-sized rat skull defect model. These combined results highlight the therapeutic potential of cell-degradable bone void fillers compared against conventional polymeric bone implants.

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Article information

Article type
Paper
Submitted
10 Oct 2024
Accepted
20 Feb 2025
First published
21 Feb 2025

Biomater. Sci., 2025, Accepted Manuscript

Oxidation-responsive, settable bone substitute composites for regenerating critically-sized bone defects

R. L. Dos Santos, A. Ahmed, B. E. Hunn, A. E. Addison, D. W. Marques, K. A. Bruce and J. Martin, Biomater. Sci., 2025, Accepted Manuscript , DOI: 10.1039/D4BM01345J

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