Polymers (Aug 2024)

Polycaprolactone—Vitamin E TPGS Micellar Formulation for Oral Delivery of Paclitaxel

  • Ziyad Binkhathlan,
  • Raisuddin Ali,
  • Osman Yusuf,
  • Abdullah H. Alomrani,
  • Mohamed M. Badran,
  • Abdullah K. Alshememry,
  • Aws Alshamsan,
  • Faleh Alqahtani,
  • Wajhul Qamar,
  • Mohamed W. Attwa

DOI
https://doi.org/10.3390/polym16152232
Journal volume & issue
Vol. 16, no. 15
p. 2232

Abstract

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This study aimed to investigate the potential of polycaprolactone–vitamin E TPGS (PCL-TPGS) micelles as a delivery system for oral administration of paclitaxel (PTX). The PCL-TPGS copolymer was synthesized using ring opening polymerization, and PTX-loaded PCL-TPGS micelles (PTX micelles) were prepared via a co-solvent evaporation method. Characterization of these micelles included measurements of size, polydispersity, and encapsulation efficiency. The cellular uptake of PTX micelles was evaluated in Caco-2 cells using rhodamine 123 (Rh123) as a fluorescent probe. Moreover, an everted rat sac study was conducted to evaluate the ex vivo permeability of PTX micelles. Additionally, a comparative pharmacokinetic study of PTX micelles versus the marketed formulation, Ebetaxel® (a Taxol generic), was performed after a single oral administration to rats. The results demonstrated that the micellar formulation significantly improved PTX solubility (nearly 1 mg/mL). The in vitro stability and release of PTX micelles in simulated gastric fluid (SGF) and simulated intestinal fluid (SIF) demonstrated that PTX micelles remained stable for up to 24 h and significantly slowed the release of PTX in both media compared to Ebetaxel®. The in vitro cellular uptake, ex vivo intestinal permeability, and in vivo pharmacokinetic profile demonstrated that PTX micelles enhanced the permeability and facilitated a rapid absorption of the drug. Conclusively, the PCL7000-TPGS3500 micelles exhibit potential as an effective oral delivery system for PTX.

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