Attension

Enhanced degradation and bioactivity in polysiloxane-based shape memory polymer (SMP) scaffolds

Year: 2023

Journal: Polymer, Volume 284, 2023-10-06, page 126291

Authors: Beltran, Felipe O.; Arabiyat, Ahmad S.; Culibrk, Robert A.; Yeisley, Daniel J.; Houk, Christopher J.; Hicks, Ashley J.; Negrón Hernández, Jenlyan; Nitschke, Brandon M.; Hahn, Mariah S.; Grunlan, Melissa A.

“Self-fitting” shape memory polymer (SMP) scaffolds based on poly(ε-caprolactone) diacrylate (PCL-DA) have the potential to improve healing of irregular bone defects due to their capacity to fill complex geometries and to intrinsically support human mesenchymal stem cell (h-MSC) mediated osteogenesis. In prior work, the incorporation of polydimethylsiloxane dimethacrylate (PDMS-DMA) resulted in PCL/PDMS SMP scaffolds that successfully induced in vitro mineralization and accelerated degradation, the latter stemming from phase separation effects. Herein, analogous scaffolds were created with a more hydrophilic polysiloxane, polymethylhydrosiloxane dimethacrylate (PMHS-DMA). When compared to analogous PCL/PDMS scaffolds, the resulting PCL/PMHS scaffolds exhibited desirably faster rates of in vitro degradation and mineralization. In vitro analyses on RGDS [Arg-Gly-Asp-Ser]-modified PCL/PMHS confirmed their capacity to intrinsically support h-MSC bone marker expression with similar specificity and potency as RGDS-containing PCL scaffolds. However, cellular spreading was reduced on RGDS-modified PCL/PMHS scaffolds versus PCL and analogous PCL/PDMS scaffolds due to a decrease in surface-available cell adhesive peptide.

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Enhanced degradation and bioactivity in polysiloxane-based shape memory polymer (SMP) scaffolds