Antagonism of Coronary Artery Relaxation by Adenosine A2A-Receptor Antagonist ZM241385
- 1 February 2000
- journal article
- research article
- Published by Wolters Kluwer Health in Journal of Cardiovascular Pharmacology
- Vol. 35 (2) , 322-325
- https://doi.org/10.1097/00005344-200002000-00022
Abstract
We have tested the existence of functional A2A adenosine receptor in porcine coronary artery using, for the first time, the new A2A antagonist ZM241385. Nonselective agonist NECA and A2A-selective agonist CGS21680 produced concentration-dependent relaxation of prostaglandin F2α (PGF2α)-precontracted endothelium intact (E+) and denuded (E−) rings. Relaxation was significantly greater in E+ rings than in E− rings. A2A adenosine receptor-selective antagonist, ZM241385 (10−6M), significantly attenuated the relaxation responses. The antagonism of ZM241385 was compared with that of SCH58261 (10−6M), another A2A adenosine receptor-selective antagonist, which also significantly attenuated the relaxation response to both agonists. However, ZM241385 produced a significantly greater shift of the relaxation-response curves to the right compared with SCH58261 both in E+ and E− rings. The data show for the first time that ZM241385 is a potent A2A-receptor antagonist in porcine coronary artery and a useful tool to study A2A-receptor function.Keywords
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