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Fabrication of Alginate-Based O/W Nanoemulsions for Transdermal Drug Delivery of Lidocaine: Influence of the Oil Phase and Surfactant
Authors:Omar Sarheed  Manar Dibi  Kanteti V. R. N. S. Ramesh  Markus Drechsler
Affiliation:1.RAK College of Pharmaceutical Sciences, RAK Medical and Health Sciences University, Ras AlKhaimah 11172, United Arab Emirates; (M.D.); (K.V.R.N.S.R.);2.Bavarian Polymer Institute, KeyLab ‘Electron & Optical Microscopy’, University of Bayreuth, 95447 Bayreuth, Germany;
Abstract:Transdermal drug delivery of lidocaine is a good choice for local anesthetic delivery. Microemulsions have shown great effectiveness for the transdermal transport of lidocaine. Oil-in-water nanoemulsions are particularly suitable for encapsulation of lipophilic molecules because of their ability to form stable and transparent delivery systems with good skin permeation. However, fabrication of nanoemulsions containing lidocaine to provide an extended local anesthetic effect is challenging. Hence, the aim of this study was to address this issue by employing alginate-based o/w nanocarriers using nanoemulsion template that is prepared by combined approaches of ultrasound and phase inversion temperature (PIT). In this study, the influence of system composition such as oil type, oil and surfactant concentration on the particle size, in vitro release and skin permeation of lidocaine nanoemulsions was investigated. Structural characterization of lidocaine nanoemulsions as a function of water dilution was done using DSC. Nanoemulsions with small droplet diameters (d < 150 nm) were obtained as demonstrated by dynamic light scattering (DLS) and cryo-TEM. These nanoemulsions were also able to release 90% of their content within 24-h through PDMS and pig skin and able to the drug release over a 48-h. This extended-release profile is highly favorable in transdermal drug delivery and shows the great potential of this nanoemulsion as delivery system.
Keywords:nanoemulsions   phase inversion temperature (PIT) method   oil type   surfactant concentration   in vitro skin permeation   pig skin   PDMS
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