ENHANCED PROSTAGLANDIN SYNTHESIS AFTER ULTRAVIOLET INJURY IS MEDIATED BY ENDOGENOUS HISTAMINE STIMULATION - A MECHANISM FOR IRRADIATION ERYTHEMA

Acute ultraviolet light B (UVB) injury is associated with dermal mast cell histamine release. The possibility that histamine-stimulated prostaglandin (PG) synthesis could be a mechanism for irradiation erythema was therefore examined using human skin explants. Explants responded to UV irradiation (120 mJ/cm2) with a fivefold increase in synthesis of prostaglandins E2, F(2α) and 6-keto PGF(1α). Incubating explants with the H1 antihistamines brompheniramine (50 μM) or pyrilamine (30 μM) inhibited PG release from irradiated explants 63 ± 4.9% (mean ± SEM) 6 h after UV exposure. Antihistamines did not affect PG synthesis in control explants. Irradiation increased the histamine concentration in explant conditioned medium only 50% over basal values, suggesting that irradiation enhanced histamine responsiveness. Explants were therefore incubated with exogenous histamine. In irradiated explants, PG synthesis was stimulated threefold by 3 μM histamine. Unirradiated explants' PG synthesis was unaffected by histamine. Enhanced histamine sensitivity was also examined in epidermal cell cultures. In irradiated cultures, histamine sensitivity was again markedly potentiated: as little as 1 μM histamine stimulated significant PGE2 release and the response to 10-30 μM histamine was increased six to eight times compared with that of unirradiated cultures. These studies demonstrate that endogenous histamine stimulates PG synthesis in human skin after UV injury by potentiation of histamine-induced prostaglandin release. Potentiated agonist responses induced by UV exposure may contribute to the effects of UVB irradiation injury and in particular to irradiation erythema.