4.7 Article

Dual-drug delivery of Ag-chitosan nanoparticles and phenytoin via core-shell PVA/PCL electrospun nanofibers

Journal

CARBOHYDRATE POLYMERS
Volume 270, Issue -, Pages -

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.carbpol.2021.118373

Keywords

Silver nanoparticles; Chitosan; Phenytoin; Dual-drug delivery; Core-shell nanofibers

Funding

  1. Islamic Development Bank (IDB) , Jeddah, Saudi Arabia [36/11207330, 23/EGT/P34]
  2. Marmara University Scientific Research Projects Coordination Unit [FENB1212180614]
  3. National Science Centre in Poland [2018/30/Q/NZ7/00281]

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Dual-drug delivery systems were constructed using coaxial techniques, showing controlled drug release and improved performance of nanofibrous membranes, which have promising applications in tissue regeneration and wound healing.
Dual-drug delivery systems were constructed through coaxial techniques, which were convenient for the model drugs used the present work. This study aimed to fabricate core-shell electrospun nanofibrous membranes displaying simultaneous cell proliferation and antibacterial activity. For that purpose, phenytoin (Ph), a well-known proliferative agent, was loaded into a polycaprolactone (PCL) shell membrane, and as-prepared silver-chitosan nanoparticles (Ag-CS NPs), as biocidal agents, were embedded in a polyvinyl alcohol (PVA) core layer. The morphology, chemical composition, mechanical and thermal properties of the nanofibrous membranes were characterized by FESEM/STEM, FTIR and DSC. The coaxial PVA-Ag CS NPs/PCL-Ph nanofibers (NFs) showed more controlled Ph release than PVA/PCL-Ph NFs. There was notable improvement in the morphology, thermal, mechanical, antibacterial properties and cytobiocompatibility of the fibers upon incorporation of Ph and Ag-CS NPs. The proposed core-shell PVA/PCL NFs represent promising scaffolds for tissue regeneration and wound healing by the effective dual delivery of phenytoin and Ag-CS NPs.

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