Influence of monoolein on progesterone transdermal delivery

Authors

  • Wanessa de Souza Cardoso Quintão University of Brasília; School of Ceilândia
  • Breno Noronha Matos University of Brasília; School of Health Sciences; Laboratory of Food, Drugs and Cosmetics
  • Thaiene Avila Reis University of Brasília; School of Health Sciences; Laboratory of Food, Drugs and Cosmetics
  • Lívia Cristina de Sá Barreto University of Brasília; School of Ceilândia
  • Taís Gratieri University of Brasília; School of Health Sciences; Laboratory of Food, Drugs and Cosmetics
  • Guilherme Msrtins Gelfuso University of Brasília; School of Health Sciences; Laboratory of Food, Drugs and Cosmetics

DOI:

https://doi.org/10.1590/S1984-82502015000400018

Abstract

This work aimed to investigate in vitro the influence of monoolein (MO) on progesterone (PG) transdermal delivery and skin retention. Information about the role of MO as an absorption enhancer for lipophilic molecules can help on innovative product development capable of delivering the hormone through the skin in a consistent manner, improving transdermal therapy of hormonal replacement. MO was dispersed in propylene glycol under heat at concentrations of 0% (control), 5% w/w, 10% w/w and 20% w/w. Then, 0.6% of PG (w/w) was added to each formulation. Permeation profile of the hormone was determined in vitro for 48 h using porcine skin in Franz diffusion cells. PG permeation doubled when 5% (w/w) of MO was present in formulation in comparison to both the control and higher MO concentrations (10% and 20% w/w). An equal trend was observed for PG retention in stratum corneum (SC) and reminiscent skin (E+D). PG release rates from the MO formulations, investigated using cellulose membranes, revealed that concentrations of MO higher than 5% (w/w) hindered PG release, which indeed negatively reflected on the hormone permeation through the skin. In conclusion, this work demonstrated the feasibility of MO addition (at 5% w/w) in formulations as a simple method to increase transdermal PG delivery for therapies of hormonal replacement. In contrast, higher MO concentrations (from 10% to 20% w/w) can control active release, and this approach could be extrapolated to other lipophilic, low-molecular-weight molecules.

Downloads

Download data is not yet available.

Downloads

Published

2015-12-01

Issue

Vol. 51 No. 4 (2015)

Section

Articles

License

All content of the journal, except where identified, is licensed under a Creative Commons attribution-type BY.

The on line journal has open and free access.

How to Cite

Influence of monoolein on progesterone transdermal delivery . (2015). Brazilian Journal of Pharmaceutical Sciences, 51(4), 923-929. https://doi.org/10.1590/S1984-82502015000400018