Antagonism of Coronary Artery Relaxation by Adenosine A2A-Receptor Antagonist ZM241385

Abstract

We have tested the existence of functional A_2A adenosine receptor in porcine coronary artery using, for the first time, the new A_2A antagonist ZM241385. Nonselective agonist NECA and A_2A-selective agonist CGS21680 produced concentration-dependent relaxation of prostaglandin F_2α (PGF_2α)-precontracted endothelium intact (E⁺) and denuded (E⁻) rings. Relaxation was significantly greater in E⁺ rings than in E⁻ rings. A_2A 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 A_2A 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 A_2A-receptor antagonist in porcine coronary artery and a useful tool to study A_2A-receptor function.