Development of a kojic monooleate-enriched oil-in-water nanoemulsion as a potential carrier for hyperpigmentation treatment

Sharifah Nurfadhlin Afifah Syed Azhar; Siti Efliza Ashari; Norazlinaliza Salim

doi:10.2147/IJN.S171532

Development of a kojic monooleate-enriched oil-in-water nanoemulsion as a potential carrier for hyperpigmentation treatment

Int J Nanomedicine. 2018 Oct 15:13:6465-6479. doi: 10.2147/IJN.S171532. eCollection 2018.

Authors

Sharifah Nurfadhlin Afifah Syed Azhar¹, Siti Efliza Ashari¹, Norazlinaliza Salim¹

Affiliation

¹ Integrated Chemical BioPhysics Research, Faculty of Science, Universiti Putra Malaysia, Serdang, Selangor, Malaysia, ctefliza@upm.edu.my.

Abstract

Introduction: Kojic monooleate (KMO) is an ester derived from a fungal metabolite of kojic acid with monounsaturated fatty acid, oleic acid, which contains tyrosinase inhibitor to treat skin disorders such as hyperpigmentation. In this study, KMO was formulated in an oil-in-water nanoemulsion as a carrier for better penetration into the skin.

Methods: The nanoemulsion was prepared by using high and low energy emulsification technique. D-optimal mixture experimental design was generated as a tool for optimizing the composition of nanoemulsions suitable for topical delivery systems. Effects of formulation variables including KMO (2.0%-10.0% w/w), mixture of castor oil (CO):lemon essential oil (LO; 9:1) (1.0%-5.0% w/w), Tween 80 (1.0%-4.0% w/w), xanthan gum (0.5%-1.5% w/w), and deionized water (78.8%-94.8% w/w), on droplet size as a response were determined.

Results: Analysis of variance showed that the fitness of the quadratic polynomial fits the experimental data with F-value (2,479.87), a low P-value (P<0.0001), and a nonsignificant lack of fit. The optimized formulation of KMO-enriched nanoemulsion with desirable criteria was KMO (10.0% w/w), Tween 80 (3.19% w/w), CO:LO (3.74% w/w), xanthan gum (0.70% w/w), and deionized water (81.68% w/w). This optimum formulation showed good agreement between the actual droplet size (110.01 nm) and the predicted droplet size (111.73 nm) with a residual standard error <2.0%. The optimized formulation with pH values (6.28) showed high conductivity (1,492.00 µScm^-1) and remained stable under accelerated stability study during storage at 4°C, 25°C, and 45°C for 90 days, centrifugal force as well as freeze-thaw cycles. Rheology measurement justified that the optimized formulation was more elastic (shear thinning and pseudo-plastic properties) rather than demonstrating viscous characteristics. In vitro cytotoxicity of the optimized KMO formulation and KMO oil showed that IC₅₀ (50% inhibition of cell viability) value was >100 µg/mL.

Conclusion: The survival rate of 3T3 cell on KMO formulation (54.76%) was found to be higher compared to KMO oil (53.37%) without any toxicity sign. This proved that the KMO formulation was less toxic and can be applied for cosmeceutical applications.

Keywords: D-optimal mixture experimental design; anti-tyrosinase; hyperpigmentation; kojic monooleate; nano-cosmeceutical.

MeSH terms

3T3 Cells
Analysis of Variance
Animals
Cell Death / drug effects
Emulsions / chemistry*
Hyperpigmentation / drug therapy*
Mice
Nanoparticles / chemistry
Nanoparticles / ultrastructure*
Oils / chemistry*
Oleic Acid / therapeutic use*
Particle Size
Pyrones / therapeutic use*
Pyrones / toxicity
Reproducibility of Results
Solubility
Time Factors
Water / chemistry*

Substances

Emulsions
Oils
Pyrones
Water
Oleic Acid
kojic acid