Topically Applied Eicosapentaenoic Acid Protects Against Local Immunosuppression Induced by UVB Irradiation, cis-Urocanic Acid and Thymidine Dinucleotides

Topically Applied Eicosapentaenoic Acid Protects Against Local Immunosuppression Induced by UVB Irradiation, cis-Urocanic Acid and Thymidine Dinucleotides

ABSTRACT UVB‐induced immunosuppression, a promoter of photocarcinogenesis, involves the formation of pyrimidine dimers and cis‐urocanic acid (cis‐UCA), but reactive oxygen species (ROS) also plays an important role. Eicosapentaenoic acid (EPA) can inhibit photocarcinogenesis, but due to its polyunsa...

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Bibliographic Details
Published in:Photochemistry and photobiology Vol. 73; no. 1; pp. 64 - 70
Main Authors: Moison, Ralf M. W., Steenvoorden, David P. T., Beijersbergen van Henegouwen, Gerard M. J.
Format: Journal Article
Language:English
Published: Oxford, UK Blackwell Publishing Ltd 01-01-2001
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Summary:ABSTRACT UVB‐induced immunosuppression, a promoter of photocarcinogenesis, involves the formation of pyrimidine dimers and cis‐urocanic acid (cis‐UCA), but reactive oxygen species (ROS) also plays an important role. Eicosapentaenoic acid (EPA) can inhibit photocarcinogenesis, but due to its polyunsaturated nature it is susceptible to oxidative damage by ROS. The antioxidant defense system may therefore be challenged upon ultraviolet‐B (UVB) irradiation in the presence of EPA. We investigated whether topically applied EPA in mice could protect against local immunosuppression (contact hypersensitivity response to dinitrofluorobenzene) induced by UVB radiation (1.5 J/cm2), or topically applied cis‐UCA (150 nmol/cm2) or thymidine dinucleotides (pTpT) (5 nmol/cm2). The influence of EPA on epidermal lipid peroxidation and antioxidant status was also measured. UVB irradiation, cis‐UCA and pTpT all caused 70% immunosuppression. Topical pretreatment of mice with EPA partially protected against immunosuppression; the EPA dose needed to accomplish this was 10 nmol/cm2 for UVB irradiation, 100 nmol/cm2 for cis‐UCA and 1000 nmol/cm2 for pTpT. Higher EPA doses caused higher UVB‐induced lipid peroxidation and lower vitamin C levels. Glutathione only decreased with the highest EPA dose whereas vitamin E was not decreased after UVB irradiation. In conclusion, topically applied EPA protects against UVB‐, cis‐UCA‐ and pTpT‐induced immunosuppression and maintenance of an adequate antioxidant defense seems to be an important prerequisite for the protective action by EPA.
Bibliography:Posted on the website on 22 November 2000.
istex:44691A90C7A5112518E424A9E5A736BD7DAD89AE
ark:/67375/WNG-LZCBTLC3-Z
ArticleID:PHP64
ISSN:0031-8655
1751-1097
DOI:10.1562/0031-8655(2001)0730064TAEAPA2.0.CO2