Please use this identifier to cite or link to this item: http://hdl.handle.net/10773/17783
Title: Development of multicore hybrid particles for drug delivery through the precipitation of CO2 saturated emulsions
Author: Gonçalves, V. S. S.
Rodríguez-Rojo, S.
Matias, A. A.
Nunes, A. V. M.
Nogueira, I. D.
Nunes, D.
Fortunato, E.
Alves de Matos, A. P.
Cocero, M. J.
Duarte, C. M. M.
Keywords: Supercritical fluids
Particles from Gas Saturated Solutions
Emulsion
Multicore hybrid particles
Drug delivery systems
Issue Date: 2015
Publisher: Elsevier
Abstract: Hybrid lipid–polymer particles are gaining increasing interest to be applied as drug delivery systems due to their greater stability in biological fluids and enhanced cellular uptake of drugs. However, a major drawback is the fact that these particles are usually produced through techniques that use organic solvents. This work studies the possibility of producing for the first time hybrid particles composed by lipid multicores enveloped in a polymeric layer through Particles from Gas Saturated Solutions (PGSS1), without using organic solvents. An oil-in-water emulsion, composed by Gelucire 43/01TM (GEL) as the discontinuous phase and by an aqueous polyethylene glycol 4000 (PEG) solution as the continuous phase, was successfully precipitated by PGSS1. Operating conditions that ensured the stability of the CO2 saturated emulsion were previously evaluated. The resulting PEG–GEL particles present a spherical-like morphology constituted by several lipid cores encapsulated into a polymeric shell. The applicability of these structured particles to be used as drug delivery system (DDS) was studied by using ketoprofen, a nonsteroidal anti-inflammatory drug (NSAID), as model drug. The particles provided an initial burst release of the drug due to the progressive dissolution of the external layer of PEG, followed by a controlled release of the NSAID from the GEL cores.
Peer review: yes
URI: http://hdl.handle.net/10773/17783
DOI: 10.1016/j.ijpharm.2014.11.003
ISSN: 0378-5173
Appears in Collections:CESAM - Artigos

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