Prostacyclin release and receptor activation: differential control of human pulmonary venous and arterial tone
- 1 June 2004
- journal article
- research article
- Published by Wiley in British Journal of Pharmacology
- Vol. 142 (4) , 788-796
- https://doi.org/10.1038/sj.bjp.0705843
Abstract
1. In human pulmonary vascular preparations, precontracted arteries were more sensitive to the relaxant effect of acetylcholine (ACh) than veins (pD(2) values: 7.25+/-0.08 (n=23) and 5.92+/-0.09 (n=25), respectively). Therefore, the role of prostacyclin (PGI(2)) was explored to examine whether this mediator may be responsible for the difference in relaxation. 2. In the presence of the cyclooxygenase (COX) inhibitor, indomethacin (INDO), the ACh relaxations were reduced in arteries but not in veins. On the contrary, an inhibitor (l-NOARG) of the nitric oxide synthase blocked preferentially the relaxation in veins. 3. A greater release of 6-keto-PGF(1alpha), the stable metabolite of PGI(2), was observed in arterial preparations than in venous preparations when stimulated with either ACh or arachidonic acid (AA). 4. Exogenous PGI(2) produced a reduced relaxant effect in the precontracted vein when compared with the artery. In the presence of the EP(1)-receptor antagonist AH6809, the PGI(2) relaxation of veins was similar to arteries. 5. In veins, AA (0.1 mm) produced a biphasic response, namely, a contraction peak (0.4-0.5 g) followed by a relaxation. These contractions in venous preparations were abolished either in the absence of endothelium or in the presence of INDO or an EP(1)-receptor antagonist (AH6809, SC19220). In the arterial preparations AA induced only relaxations. 6. In both vascular preparations, COX-1 but not the COX-2 protein was detected in microsomal preparations derived from homogenized tissues or freshly isolated endothelial cells. 7. The differential vasorelaxations induced by ACh may be explained, in part, by a more pronounced production and release of PGI(2) in human pulmonary arteries than in the veins. In addition, while PGI(2) induced relaxation by activation of IP-receptors in both types of vessels, a PGI(2) constrictor effect was responsible for masking the relaxation in the veins by activation of the EP(1)-receptor.Keywords
This publication has 60 references indexed in Scilit:
- TNF‐α, inefficient by itself, potentiates IL‐1β‐induced PGHS‐2 expression in human pulmonary microvascular endothelial cells: requirement of NF‐κB and p38 MAPK pathwaysBritish Journal of Pharmacology, 2002
- Prostanoid receptors involved in the relaxation of human pulmonary vesselsBritish Journal of Pharmacology, 1999
- Mediators of Arachidonic Acid–Induced Relaxation of Bovine Coronary ArteryHypertension, 1996
- Peroxynitrite formed by simultaneous generation of nitric oxide and superoxide selectively inhibits bovine aortic prostacyclin synthaseFEBS Letters, 1996
- Prostacyclin synthesis in ovine pulmonary artery is developmentally regulated by changes in cyclooxygenase-1 gene expression.Journal of Clinical Investigation, 1994
- Tone dependent nitric oxide production in ovine vessels in vitroRespiration Physiology, 1993
- Prostaglandin H2 may be the endothelium-derived contracting factor released by acetylcholine in the aorta of the rat.Hypertension, 1990
- Difference between Endothelium-Dependent Relaxation in Arterial and in Venous Coronary Bypass GraftsNew England Journal of Medicine, 1988
- The obligatory role of endothelial cells in the relaxation of arterial smooth muscle by acetylcholineNature, 1980
- Human Pulmonary Endothelial Cells in CultureJournal of Clinical Investigation, 1980