4.7 Article

Enhancement. of follicular delivery of finasteride by liposomes and niosomes -: 1.: In vitro permeation and in vivo deposition studies using hamster flank and ear models

Journal

INTERNATIONAL JOURNAL OF PHARMACEUTICS
Volume 323, Issue 1-2, Pages 1-10

Publisher

ELSEVIER
DOI: 10.1016/j.ijpharm.2006.05.041

Keywords

finasteride deposition in the pilosebaceous units; niosomes; liposomes; skin permeation; hamster; follicular drug delivery

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Finasteride is indicated orally in the treatment of androgenetic alopecia and some other pilosebaceous unit (PSU) disorders. We wished to investigate whether topical application of finasteride-containing vesicles (liposomes and niosomes) could enhance drug concentration at the PSU, as compared to finasteride hydroalcoholic solution (HA). Liposomes consisted of phospholipid (dimyristoyl phosphatidylcholine (DMPC) or egg lecithin): cholesterol: dicetylphosphate (8:2:1, mole ratio). Niosomes were comprising non-ionic surfactant (polyoxyethylene alkyl ethers (Brij (R) series) or sorbitan monopalmitate): cholesterol: dicetylphosphate (7:3:1, mole ratio). Vesicles were prepared by the film hydration technique and characterized with regard to the size, drug entrapment efficiency and gel-liquid transition temperature (T-c) In vitro permeation of H-3-finasteride through hamster flank skin was faster from hydroalcoholic solution (0.13 mu g/cm(2) h) compared to vesicles (0.025-0.058 mu g/cm(2) h). In vivo deposition of H-3-finasteride vesicles in hamster ear showed that liquid-state vesicle, i.e. those made of DMPC or Brij97:Brij76 (1:1), were able to deposit 2.1 or 2.3% of the applied dose to the PSU, respectively. This was significantly higher than drug deposition by gel-state vesicles (0.35-0.51%) or HA (0.76%). Both in vitro permeation and in vivo deposition studies, demonstrated the potentials of liquid-state liposomes and niosomes for successful delivery of finasteride to the PSU. (c) 2006 Elsevier B.V. All rights reserved.

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