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Shape memory cycle conditions impact human bone marrow stromal cell binding to RGD- and YIGSR-conjugated poly (glycerol dodecanedioate). | LitMetric

AI Article Synopsis

  • Bioresorbable shape memory polymers (SMPs) like poly(glycerol dodecanedioate) (PGD) offer potential solutions for minimally invasive surgeries by facilitating tissue repair, but they require biocompatibility through the incorporation of bioactive ligands.
  • In this study, specific cell-adhesive peptides (RGD and YIGSR) were conjugated to PGD, enhancing cell attachment and proliferation, particularly when both peptides were used together compared to single peptide applications.
  • Results indicate that the shape memory cycle conditions affect the functionality and specificity of the peptides, with the arrangement of these peptides after recovery influencing their effectiveness in promoting cell binding, which is crucial for designing functionalized

Article Abstract

Bioresorbable shape memory polymers (SMP) are an emerging class of polymers that can help address several challenges associated with minimally invasive surgery by providing a solution for structural tissue repair. Like most synthetic polymer networks, SMPs require additional biorelevance and modification for biomedical applications. Methodologies used to incorporate bioactive ligands must preserve SMP thermomechanics and ensure biofunctionality following in vivo delivery. We have previously described the development of a novel thermoresponsive bioresorbable SMP, poly (glycerol dodecanedioate) (PGD). In this study, cell-adhesive peptide sequences RGD and YIGSR were conjugated with PGD. We investigated 1) the impact of conjugated peptides on the fixity (R), recovery (R), and recovery rate (dR/dT), 2) the impact of conjugated peptides on cell binding, and 3) the impact of the shape memory cycle (T) on conjugated peptide functionality towards binding human bone marrow stromal cells (BMSC). Peptide conjugation conditions impact fixity but not the recovery or recovery rate (p < 0.01). Peptide-conjugated substrates increased cell attachment and proliferation compared with controls (p < 0.001). Using complementary integrin binding cell-adhesive peptides increased proliferation compared with using single peptides (p < 0.05). Peptides bound to PGD substrates exhibited specificity to their respective integrin targets. Following the shape memory cycle, peptides maintained functionality and specificity depending on the shape memory cycle conditions (p < 0.001). The dissipation of strain energy during recovery can drive differential arrangement of conjugated sequences impacting functionality, an important design consideration for functionalized SMPs. STATEMENT OF SIGNIFICANCE: Shape memory elastomers are an emerging class of polymers that are well-suited for minimally invasive repair of soft tissues. Tissue engineering approaches commonly utilize biodegradable scaffolds to deliver instructive cues, including cells and bioactive signals. Delivering these instructive cues on biodegradable shape memory elastomers requires modification with bioactive ligands. Furthermore, it is necessary to ensure the specificity of the ligands to their biological targets when conjugated to the polymer. Moreover, the bioactive ligand functionality must be conserved after completing the shape memory cycle, for applications in tissue engineering.

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Source
http://dx.doi.org/10.1016/j.actbio.2024.07.057DOI Listing

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