Effects of adenosine receptor agonists on guinea-pig isolated working hearts and the role of endothelium and NO

The hypothesis that the coronary vasodilator effects of adenosine receptor agonists are independent of the vascular endothelium or mediators derived therefrom was examined in guinea‐pig isolated working hearts. Adenosine receptor agonists, 5′‐(N‐ethylcarboxamido)‐adenosine (NECA; two‐fold selective...

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Bibliographic Details
Published in:Journal of pharmacy and pharmacology 2002-06, Vol.54 (6), p.859-867
Main Authors: Maddock, Helen L, Broadley, Kenneth J, Bril, Antoine, Khandoudi, Nassirah
Format: Article
Language:English
Subjects:
Adenosine - analogs & derivatives
Adenosine - pharmacology
Animals
Antianginal agents. Coronary vasodilator agents
Biological and medical sciences
Cardiovascular system
Cyclooxygenase Inhibitors - pharmacology
Endothelium, Vascular - drug effects
Endothelium, Vascular - physiology
Guinea Pigs
Heart - drug effects
Heart - physiology
Hemodynamics - drug effects
In Vitro Techniques
Indomethacin - pharmacology
Male
Medical sciences
Nitric Oxide - metabolism
Nitric Oxide Synthase - antagonists & inhibitors
Pharmacology. Drug treatments
Phenethylamines - pharmacology
Prostaglandins - metabolism
Purinergic P1 Receptor Agonists
Triazines - pharmacology
Triazoles - pharmacology
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Summary:The hypothesis that the coronary vasodilator effects of adenosine receptor agonists are independent of the vascular endothelium or mediators derived therefrom was examined in guinea‐pig isolated working hearts. Adenosine receptor agonists, 5′‐(N‐ethylcarboxamido)‐adenosine (NECA; two‐fold selective for A2 over A1 receptors), 2‐[p‐(2‐carboxyethyl)phenylethylamino]‐5′‐N‐ethylcarboxamidoadenosine (CGS21680; A2A selective), N6‐cyclopentyl‐adenosine (CPA; A1 selective) and N6‐(3‐iodobenzyl)adenosine‐5′‐N‐methyluronamide (IB‐MECA; A3 selective), were infused (3 times 10−7 M) after endothelium removal by passing oxygen through the coronary circulation. In spontaneously beating hearts, CGS21680 and NECA increased, while CPA decreased, coronary flow. NECA and CPA reduced heart rate, left ventricular pressure and aortic output. The nitric oxide synthase (NOS) inhibitor, NG‐nitro‐L‐arginine (L‐NOARG; 3 times 10−5 M) abolished the vasodilatation by NECA but not CGS21680, indicating that nitric oxide (NO) of a non‐endothelial source mediated the NECA response. Coronary vasodilatation by CGS21680 was inhibited by the A2A receptor antagonist, 4‐(2‐[7‐amino‐2‐(2‐furyl)[1,2,4]triazolo [2,3‐a][1,3,5]triazin‐5‐ylamino]ethyl)phenol (ZM241385). Indometacin (10−6 M) attenuated the coronary vasodilatation to CGS21680, suggesting a partial role for cyclooxygenase products. IBMECA had no effect, indicating no A3 receptor involvement. In paced working hearts, the responses were similar except CPA had no effect on coronary flow or aortic output and CGS21680 increased left ventricular pressure and the maximum rate of ventricular pressure rise. This study has demonstrated functionally effective removal of the endothelium by a novel method of passing oxygen through the coronary vasculature. A coronary vasodilator action of adenosine receptor agonists mediated via A2A receptors is endothelium‐and NO‐independent, but partially involves cyclooxygenase products.
ISSN:0022-3573
2042-7158
DOI:10.1211/0022357021779041