4.4 Article

Autoclaving of Poloxamer 407 hydrogel and its use as a drug delivery vehicle

Publisher

WILEY
DOI: 10.1002/jbm.b.34703

Keywords

autoclave; drug delivery; hydrogel; Poloxamer 407; sterilization

Funding

  1. Mississippi State University's Bagley College of Engineering Undergraduate Research Stipend
  2. Mississippi State University's Department of Clinical Sciences in the College of Veterinary Medicine
  3. NIH [P20GM103646-07]
  4. Mississippi State University's Office of Research and Economic Development

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Autoclaving decreased the water content and gelation temperature of P407 hydrogel, but did not affect its rheological properties and efficacy as a drug delivery vehicle for vancomycin.
With antibiotic-resistant bacteria becoming increasingly prevalent, biomaterials capable of targeted, in situ drug delivery are urgently needed. The synthetic polymer Poloxamer 407 (P407) is of particular interest due to its thermoreversible gelation. Clinical use of P407 typically involves sterilization via autoclaving, but the effects of these extreme environmental conditions on hydrogel water content, rheological properties and efficacy as a drug delivery vehicle remain unknown. The aim of this study was to investigate the effects of autoclaving on the properties of P407 hydrogel. Autoclaving reduced hydrogel water content due to evaporation, thus increasing the polymer weight fraction of the hydrogels. In contrast, except for a reduction in gelation temperature following autoclaving, autoclaved hydrogels had similar rheological properties as nonautoclaved hydrogels. In vitro, autoclaving did not hinder the hydrogel's efficacy as a carrier for vancomycin antibiotic, and P407 (with and without vancomycin) had a bactericidal effect on planktonicStaphylococcus aureus. An in vivo pilot study using P407 to deliver bacteriophage highlighted the need for additional understanding of the functionality of the hydrogel for surgical applications. In conclusion, P407 hydrogel water content and gelation temperature were reduced by autoclave sterilization, while other rheological properties and the efficacy of the biomaterial as a delivery vehicle for vancomycin in vitro were unaffected.

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