• Title of article

    Preparation and optimization of polymeric micelles as an oral drug delivery system for deferoxamine mesylate: in vitro and ex vivo studies

  • Author/Authors

    Salimi ، Anayatollah - Ahvaz Jundishapur University of Medical Sciences , Sharif Makhmal Zadeh ، Behzad - Ahvaz Jundishapur University of Medical Sciences , Kazemi ، Moloud - Ahvaz Jundishapur University of Medical Sciences

  • Pages
    15
  • From page
    293
  • To page
    307
  • Abstract
    Deferoxamine mesylate (DFO) is administered as a slow subcutaneous or intravenous infusion due to its poor oral bioavailability and lack of dose proportionality. The aim of the present study was to prepare and optimize polymeric micelles containing DFO, as an oral drug delivery system for increasing permeability and oral bioavailability. Based on a full factorial design with three variables in two levels, eight polymeric micelle formulations were made using film hydration method. Two polymers including 0.1% of carbomer 934 and Poloxamer® P 407 and two blends of surfactant + co-surfactant including 1 and 2 fold of critical micelle concentration of Labrafil® + Labrasol® and Tween 80 + Span 20 were used to prepare polymeric micelles. The effect of variables on particle size (PS), entrapment efficiency (EE), drug release, thermal behavior, in vitro iron bonding and ex vivo rat intestinal permeability were evaluated. The PS of polymeric micelles was less than 83 nm that showed 80% EE with continuous drug release pattern. The change in type of polymer from carbomer to Ploxamer® significantly increased drug release. All polymeric micelles increased the iron-bonding ability of DFO compared to control. This could be due to surfactants that can play an important role in this ability. Polymeric micelles increased drug permeability through intestine more than 2.5 folds compared to control mainly affected by polymer type. Optimized polymeric micelle consists of Tween 80 and Span 20 with 1.35 folds of critical micelle concentration and Poloxamer® demonstrated 97.32% iron bonding and a 3-fold increase in permeation through the rat intestine compared with control.
  • Keywords
    Deferoxamine mesylate , Iron chelators , Oral bioavailability , Polymeric micelle , Thalassemia
  • Journal title
    Research in Pharmaceutical Sciences
  • Serial Year
    2019
  • Journal title
    Research in Pharmaceutical Sciences
  • Record number

    2465597