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Surfactants from itaconic acid: Toxicity to HaCaT keratinocytes in vitro, micellar solubilization, and skin permeation enhancement of hydrocortisone

Authors :
Mireia Broch Gosser
Angela Abruzzo
Teresa Cerchiara
David M. Brown
Barbara Luppi
Nicola Armenise
Federica Bigucci
Teresa F. Fernandes
Helinor Jane Johnston
Paola Galletti
Emilio Tagliavini
Chiara Samorì
Abruzzo, Angela
Armenise, Nicola
Bigucci, Federica
Cerchiara, Teresa
Gösser, Mireia Broch
Samorì, Chiara
Galletti, Paola
Tagliavini, Emilio
Brown, David M.
Johnston, Helinor J.
Fernandes, Teresa F.
Luppi, Barbara
Source :
International Journal of Pharmaceutics. 524:9-15
Publication Year :
2017
Publisher :
Elsevier BV, 2017.

Abstract

One of the most widely used approaches for improving drug permeation across the stratum corneum barrier of the skin is the use of chemical penetration enhancers, such as surfactants. In this study, two anionic surfactants, named C12-OPK and C18-OPK, were synthesized via condensation of itaconic acid and fatty amines, with C12 and C18 alkyl chains, respectively. Assessment of impacts on HaCaT keratinocyte cell viability was used as indicator of their potential to cause skin irritation 24 h post exposure (Alamar Blue assay). The LC50 values of C12-OPK and C18-OPK (144 and 85 mg/L, respectively) were lower than LC50 values of the most used commercial surfactants (e.g. SDS). The effect of different surfactant concentrations (up to ten times the critical micellar concentration, CMC) on hydrocortisone (HC) solubility and permeation through porcine skin was also evaluated. Results showed that drug solubility increased linearly with increasing concentrations of both surfactants, as a consequence of the association between drug and micelles. In vitro permeation results showed that the permeability coefficient increased at surfactant concentrations lower than the CMC. In particular, a higher enhancement effect on drug permeation was obtained with C18-OPK, due to its hydrophobic properties that ensured a more effective HC permeation in comparison to C12-OPK.

Details

ISSN :
03785173
Volume :
524
Database :
OpenAIRE
Journal :
International Journal of Pharmaceutics
Accession number :
edsair.doi.dedup.....53c9bdc69a66b8a246b179600b53dfec
Full Text :
https://doi.org/10.1016/j.ijpharm.2017.03.056