Pharmacology of RALGA, a mixture of retinaldehyde and glycolic acid

Christian Tran; Behrooz Kasraee; Denise Grand; Pierre Carraux; Liliane Didierjean; Olivier Sorg; Jean-Hilaire Saurat

doi:10.1159/000082542

Pharmacology of RALGA, a mixture of retinaldehyde and glycolic acid

Dermatology. 2005:210 Suppl 1:6-13. doi: 10.1159/000082542.

Authors

Christian Tran¹, Behrooz Kasraee, Denise Grand, Pierre Carraux, Liliane Didierjean, Olivier Sorg, Jean-Hilaire Saurat

Affiliation

¹ Department of Dermatology, University Hospital, Geneva, Switzerland. christian.tran@hcuge.ch

PMID: 15724102
DOI: 10.1159/000082542

Abstract

Background: Retinoids and alpha-hydroxy acids (AHAs) are major compounds in topical therapy. They exert distinct but potentially complementary activities. However, their association is limited by their respective irritating potential. Recently, the first association between a retinoid and an AHA has been achieved; this formulation (RALGA) associates retinaldehyde (RAL)--a precursor of retinoic acid (RA)--and glycolic acid (GA)--an AHA.

Objective: To study the pharmacological properties of RALGA.

Methods: The bioavailability of RAL into the skin after topical RALGA was studied by HPLC, and its bioconversion to RA was analysed by measuring the enzyme activity of retinaldehyde dehydrogenase and the RA content in the epidermis and dermis. The retinoid activity of RALGA was studied on the modulation of Hhb4 keratin mRNA on the tail of C57BL/6 mice, and its comedolytic properties on the size and density of dermal cysts and the morphology of sebaceous glands in hairless mice.

Results: Epidermal and dermal concentrations of RAL and RA were higher after RALGA treatment, as compared to both RAL 0.1% alone and RA 0.05% alone; this indicates that the presence of GA favours the bioavailability and biotransformation of RAL into RA. The retinoid activity of RALGA (suppression of Hhb4 mRNA keratin) was similar to that of RAL alone, indicating that the presence of GA does not interfere with specific retinoid activity; GA alone had no effect in this test, which confirms the specificity of Hhb4 mRNA keratin modulation for retinoid activity. The diameter and the density of dermal cysts as well as the size of sebaceous glands were significantly decreased by RALGA.

Conclusion: These observations indicate that the addition of an AHA such as GA to a retinoid such as RAL results in a better bioavailability of the retinoid, thus a higher delivery of RA, which potentiates the biological activities of the retinoid. This combination allows a delivery of high amounts of RA in the skin while preventing the side-effects usually observed with high concentrations of topical RA.

Publication types

Comparative Study

MeSH terms

Aldehyde Oxidoreductases / analysis
Animals
Biological Availability
Biotransformation
Chromatography, High Pressure Liquid
Cysts / drug therapy
Dermatologic Agents / pharmacokinetics
Dermatologic Agents / pharmacology*
Dermis / enzymology
Dermis / metabolism
Drug Combinations
Epidermis / enzymology
Epidermis / metabolism
Female
Glycolates / pharmacokinetics*
Glycolates / pharmacology*
Keratins / drug effects
Keratolytic Agents / pharmacokinetics
Keratolytic Agents / pharmacology*
Mice
Mice, Hairless
Mice, Inbred C57BL
Mice, Inbred Strains
Retinal Dehydrogenase
Retinaldehyde / pharmacokinetics*
Retinaldehyde / pharmacology*
Sebaceous Glands / drug effects
Tretinoin / analysis

Substances

Dermatologic Agents
Drug Combinations
Glycolates
Keratolytic Agents
diacneal
glycolic acid
Tretinoin
Keratins
Aldehyde Oxidoreductases
Retinal Dehydrogenase
Retinaldehyde