par Ghaffari Bohlouli, Pejman 
;Siminska-Stanny, Julia ;Jafari, Hafez ;Mirzaei, Mahta ;Nie, Lei;Delporte, Christine ;Shavandi, Armin
Référence International journal of biological macromolecules, 232, 123348
Publication Publié, 2023-01-01
;Siminska-Stanny, Julia ;Jafari, Hafez ;Mirzaei, Mahta ;Nie, Lei;Delporte, Christine ;Shavandi, Armin Référence International journal of biological macromolecules, 232, 123348
Publication Publié, 2023-01-01
Article révisé par les pairs
| Résumé : | Targeted delivery of bioactive agents, growth factors, and drugs to skin wounds is a growing trend in biomaterials development for wound healing. This study presents a printable hyaluronic acid (HA) based hydrogel to deliver yeast-derived ACE-inhibitory peptide of VLSTSFPPW (VW-9) to the wound site. We first conjugated tyramine (Ty) on the carboxyl groups of the HA to form a phenol-functionalized HA (HA-Ty); then, the carboxylic acid groups of HA-Ty were aminated with ethylenediamine (HA-Ty-NH2). The primary amine groups of the HA-Ty-NH2 could then react with the carboxylic acids of the peptide. The hydrogel was then 3D printed and crosslinked with visible light. The modification of HA was confirmed by 1H NMR and FTIR. The swelling capacity of the conjugated hydrogels was 1.5-fold higher compared to the HA-Ty-NH2 hydrogel. The conjugated peptide did not affect on rheological properties and morphology of the hydrogels. The 3T3-L1 fibroblast cells seeded on the peptide-modified hydrogels exhibited higher viability than the hydrogels without the peptide, indicating that the peptide-enriched hydrogels may have the potential for wound healing applications. |
