1. Ultraviolet-B-Induced Erythema is Mediated by Nitric Oxide and Prostaglandin E[sub 2] in Combination.
- Author
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Rhodes, L. E., Belgi, G., Parslew, R., McLoughlin, L., Clough, G. F., and Friedmann, P. S.
- Subjects
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ULTRAVIOLET radiation , *ERYTHEMA , *NITRIC oxide , *PROSTAGLANDINS E , *THERAPEUTICS - Abstract
Ultraviolet-B-induced erythema (one, two, or four times the minimal erythema dose) was reduced but not abolished by application of 1% indomethacin gel immediately after irradiation of human skin. Continuous synthesis of prostaglandins is reflected by similar levels of indomethacin-mediated inhibition of erythema at any time within 48 h after irradiation. Repeated applications of indomethacin did not increase the inhibition. Twenty-four hours after irradiation with four minimal erythema doses, mean prostaglandin E[sub 2] levels in suction blisters were 27.2 ng per ml (SEM 11) compared with 8.6 ng per ml in unirradiated skin (n = 25; p < 0.01). Prosta glandin E[sub 2] levels in dermal tissues, sampled by microdialysis (depth 0.6 ± 0.1 mm), were 310 pg per ml (SEM 123) and 237 pg per ml (SEM 88) in irradiated and unirradiated skin, respectively (n = 7, n.s.). Nitric oxide also made a significant contribution to ultraviolet-B-induced erythema. Ultraviolet erythema was inhibited by L-NAME in a dose-related fashion with 2 mM L-NAME causing total abolition of the response. L-NAME was effective at all time points up to 48 h suggesting that NO was produced continuously. NO was undetectable in suction blister fluid but in dermal microdialysate NO was present at 44.3 ng per ml (SEM 6.2) following ultraviolet B compared with 26.0 ng per ml (SEM 8.0) in unirradiated skin (p < 0.05), approximately 1000 times the molar concentration of prostaglandin E[sub 2]. These findings confirm prostaglandin E[sub 2] and NO to be mediators of ultraviolet-induced erythema. They also show that there is prolonged synthesis of both mediators within the erythemal response and that synthesis of NO is induced by lower doses of ultraviolet B compared with that of prostaglandin E[sub 2]. [ABSTRACT FROM AUTHOR]
- Published
- 2001
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