Özet
In this study, minocycline-imprinted hydrogels are developed for controlled drug delivery in ocular disease treatments. An integrated computational and experimental study are conducted for investigating the relationship between design parameters and the drug loading/release performance of hydrogels. First, suitable functional monomers are determined for successful drug-imprinting by studying pre-polymerization conditions with full-atom molecular dynamics (MD) simulations. MD simulations suggest that acrylic acid and itaconic acid are suitable monomers for imprinting minocycline. Then, minocycline-imprinted hydrogels are synthesized with acrylic acid, commonly used in hydrogels, and three different amounts of cross-linker ethylene glycol dimethacrylate, 1, 2 and 3 mol%. All hydrogels are characterized and their drug loading and release performances are determined. Our computational and experimental calculations indicate an optimum cross-linker amount of 2 mol% for controlled minocycline release from imprinted hydrogels with an imprinting factor of almost 3. Finally, the drug release kinetics are determined by Korsmeyer-Peppas model.
| Orijinal dil | İngilizce |
|---|---|
| Makale numarası | 258 |
| Dergi | Journal of Polymer Research |
| Hacim | 25 |
| Basın numarası | 12 |
| DOI'lar | |
| Yayın durumu | Yayınlandı - 1 Ara 2018 |
Bibliyografik not
Publisher Copyright:© 2018, Springer Nature B.V.
Finansman
Acknowledgments This work was supported by Scientific Research Project Coordination Unit of Istanbul University [project number ITU BAP 38271]. The authors acknowledge Dr. Ozlem Gurses (Dunya Goz Hospital, Ankara, Turkey) for her comments and valuable suggestions about the treatment of corneal neovascularization.
| Finansörler | Finansör numarası |
|---|---|
| Istanbul Üniversitesi | ITU BAP 38271 |
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