Effect of nicotine on the formation of prostacyclin‐like activity and thromboxane in rabbit aorta and platelets

Abstract

1 The effect of nicotine on the bioformation of prostacyclin (PGI₂) and of thromboxane (Tx)B₂ in rabbit aorta and platelets, respectively, was investigated. 2 Rabbit aortic rings were incubated with [¹⁴C]-arachidonic acid ([¹⁴C]-AA) and the incubation products were separated with thin layer chromatography (t.l.c). Alternatively, the aortic rings were incubated without substrate and their spontaneous formation of platelet anti-aggregatory activity was measured. Rabbit platelet microsomes were incubated with [¹⁴C]-AA and the products formed were separated with t.l.c. 3 Rings of aorta were found to be incapable of converting added [¹⁴C]-AA to labelled 6-keto-PGF_1α (the stable hydrolysis product of PGI₂). Rings of aorta incubated in saline medium spontaneously formed PGI₂-like activity. This formation was dose-dependently inhibited by nicotine, with an I₅₀ of about 10⁻⁴ m. 4 Platelet microsomes converted [¹⁴C]-AA to labelled TxB₂. This formation was unaffected by nicotine. 5 It is concluded that a true difference in sensitivity to nicotine exists between cyclo-oxygenase in rabbit aorta and platelets. The data also demonstrate a tissue difference between rabbit aorta and platelets concerning their utilization of exogenous AA as substrate in the formation of platelet active compounds.