PARALLEL OBSERVATION OF THE OCCUPANCY OF THE ALPHA-2-ADRENERGIC RECEPTOR IN INTACT PLATELETS AND ITS ABILITY TO INHIBIT THE ADENYLATE-CYCLASE
- 1 January 1982
- journal article
- research article
- Vol. 22 (3) , 574-579
Abstract
The binding of the selective .alpha.2-adrenergic receptor antagonist [methyl-3H]yohimbine to intact human blood platelets was studied in parallel with an assessment of the ability of epinephrine to inhibit their accumulation of cAMP in response to prostaglandin E1 and a phosphodiesterase inhibitor. Specifically bound [3H]yohimbine dissociated in a monoexponential fashion, and equilibrium binding showed 200-400 site/platelet with a dissociation constant of 2-7 nM. The concentration of epinephrine which inhibited cAMP accumulation was 1/4 of that required for an equal degree of inhibition of [3H]yohimbine binding. The concentration of yohimbine required to inhibit the action of epinephrine on the adenylate cyclase was 10 times higher than that required for an equal degree of saturation of the .alpha.2-adrenoreceptor. The ability of epinephrine and the partial agonist p-aminoclonidine to compete with [3H]yohimbine for binding was not influenced by agonist-occupation of the ADP receptor, which also inhibits the adenylate cyclase. These results are not compatible with the concept that each adenylate cyclase unit is coupled to an .alpha.2-receptor, nor do they indicate that the agonist-occupied .alpha.2-receptor forms a complex with the enzyme which persists for the duration of the inhibitory effect. A persistent inhibition of the cyclase is apparently induced by a brief interaction between the agonist-occupied receptor and the adenylate cyclase.This publication has 10 references indexed in Scilit:
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