Muscarinic cholinergic-receptor stimulation of specific GTP hydrolysis related to adenylate cyclase activity in canine cardiac sarcolemma.

Author:

Fleming J W1,Watanabe A M1

Affiliation:

1. Department of Pharmacology and Toxicology, Indiana University School of Medicine, Indianapolis.

Abstract

One component of muscarinic receptor inhibition of the function of cardiac ventricles is mediated by the inhibition of activated adenylate cyclase activity in sarcolemma. We have shown previously that muscarinic agonists inhibit GTP- but not Gpp(NH)p-activated adenylate cyclase activity, and various studies in other tissues indicate that nonhydrolyzable GTP analogues prevent inactivation of the enzyme. These data have suggested a role for GTP hydrolysis in the mechanism of inhibition of adenylate cyclase. The present study demonstrates that purified canine cardiac sarcolemma displays high-affinity GTPase activity that is reciprocally related to adenylate cyclase activity. The high-affinity GTPase activity was stimulated by muscarinic agonists and blocked by atropine. Furthermore, the one-half maximal effects of oxotremorine for binding to muscarinic receptors, stimulation of high-affinity GTPase activity, and inhibition of adenylate cyclase activity were similar. Muscarinic stimulation of GTPase activity and inhibition of adenylate cyclase activity required functional activity of the pertussis toxin (IAP) substrate(s). Treatment of sarcolemmal membranes with IAP attenuated the ability of oxotremorine to both stimulate high-affinity GTPase activity and inhibit adenylate cyclase activity. These studies indicate that muscarinic receptor stimulation of high-affinity GTPase activity dependent on functional IAP substrate(s) is closely linked to the mechanism of muscarinic inhibition of adenylate cyclase activity.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine,Physiology

Reference64 articles.

1. Watanabe AM: Cholinergic agonists and antagonists in Rosen MR Hoffman BF (eds): Cardiac Therapy. The Hague Martinus Nyhoff 1983 pp 95-144

2. Adenyl cyclase: III. The effect of catecholamines and choline esters on the formation of adenosine 3',5'-phosphate by preparations from cardiac muscle and liver;Murad F;J Biol Chem,1962

3. Watanabe AM: Cellular mechanisms of muscarinic regulation of cardiac function in Randall W (ed): Nervous Control of Cardiac Function. New York Oxford University Press 1984 pp 130-164

4. Mechanisms of muscarinic modulation of protein phosphorylation in intact ventricles;Watanabe AM;Fed Proc,1984

5. G proteins and dual control of adenylate cyclase

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