The action of prostanoid receptor agonists and antagonists on smooth muscle and platelets

Abstract

1 Prostanoid receptors have been characterized in a range of guinea-pig and rat smooth muscle and platelets, according to the scheme of Coleman et al., (1985a), using agonists (prostaglandin D₂ (PGD₂), PGE₁, PGE₂, 16,16 dimethyl PGE₂, PGF_2α, PGI₂ and U46619) and putative selective antagonists (AH 6809 and SQ 29,548). 2 The ileum possesses EP₁- and IP-receptors; the trachea, EP₁-EP₂- and TP-receptors; the oesophageal muscularis mucosa, EP₁- and TP-receptors; the aorta and the portal vein TP-receptors. The rat colon possesses IP-, FP- and TP-receptors. 3 Guinea-pig platelets possess both IP and DP receptors mediating an inhibition of aggregation and TP receptors mediating proaggregation responses. No evidence was found for the presence of EP₁-, EP₂- or FP-receptors. 4 Misoprostol and fenprostalene were characterized using the above preparations. Misoprostol acts as a selective EP₁-agonist, and has little or no DP, FP, IP and TP activity. In the trachea precontracted with carbachol no evidence of EP₂-receptor stimulation was observed. Fenprostalene possesses FP and TP activity but no EP₁, EP₂, DP or IP activity.