Effect of endothelium removal on stimulatory and inhibitory modulation of rat aortic prostacyclin synthesis

Abstract

1 Removal of the endothelium (DE) enhanced the in vitro release of prostacyclin (PGI₂) by rat aortae in response to adrenaline (Ad), noradrenaline (NA), thromboxane A₂ analogue U46619, phorbol dibutyrate (PDBU) and sodium fluoride (NaF) when assessed at 3 h post DE. At 6 h post DE, there were no differences between the dose-response curves obtained from aortic rings with or without endothelium. 2 At 3 h post DE the antagonism of Ad- and NA-stimulated PGI₂ synthesis by yohimbine and prazosin, and NA-stimulated PGI₂ synthesis by nifedipine was markedly reduced in aortae without eudothelium when compared with controls. These effects were reversed by protracted incubation of aortic tissue post DE (6 h and 9 h). 3 Acetylcholine, carbachol, substance P and nitroprusside were without effect on de novo or NA-stimulated PGI₂ synthesis, whether or not the endothelium was present and irrespective of incubation time, post-DE. 4 These results indicate that: (a) PGI₂ synthesis linked to excitatory receptors (α-adrenoceptors, thromboxane A₂) and associated systems (G proteins, protein kinase C) in the smooth muscle component of the rat aorta is not influenced by endothelium-derived relaxing factor (EDRF); (b) the changes of response to stimulators and inhibitors of PGI₂ synthesis may be due to an increased reactivity of the vessels caused by the trauma of DE; and (c) vasodilators (parasympathomimetics, substance P and nitroprusside) that do not act directly on excitatory receptors do not influence PGI₂ synthesis.