Hormonal inhibition of adenylate cyclase. α2 Adrenergic receptors promote release of [3H]guanylylimidodiphosphate from platelet membranes | Health & Environmental Research Online (HERO)

HERO ID

8352142

Reference Type

Journal Article

Title

Hormonal inhibition of adenylate cyclase. α2 Adrenergic receptors promote release of [3H]guanylylimidodiphosphate from platelet membranes

Author(s)

Michel, T; Lefkowitz, RJ

Year

1982

Is Peer Reviewed?

Yes

Journal

Journal of Biological Chemistry
ISSN: 0021-9258
EISSN: 1083-351X

Volume

257

Issue

22

Page Numbers

13557-13563

Language

English

Abstract

Human platelet membranes contain α2 adrenergic receptors which mediate the guanine nucleotide-dependent inhibition of adenylate cyclase induced by epinephrine. Previous investigations have provided insight into the mechanisms of adenylate cyclase stimulation by studying hormone-induced release of radiolabeled guanine nucleotides from membranes preincubated with the nucleotides. In the present studies, we demonstrate that epinephrine promotes the release of [3H]guanylylimidodiphosphate ([3H]Gpp(NH)p) from prelabeled human platelet membranes. The effect of epinephrine is α2 adrenergic in nature and requires the presence of GTP. The maximal amount of [3H]Gpp(NH)p released by epinephrine, 328 ± 29 fmol/mg of membrane protein (mean ± S.E., n = 33), is similar to the number of platelet membrane α2 adrenergic receptors determined by radioligand binding studies. Partial α2 adrenergic agonists release a smaller fraction of [3H]Gpp(NH)p than does the full agonist epinephrine. There is a significant correlation between an adrenergic agonist's intrinsic activity for adenylate cyclase inhibition and its intrinsic activity for stimulation of [3H]Gpp(NH)p release. Prostaglandin E1 (PGE1), which stimulates adenylate cyclase activity in these platelet membranes, also promotes release of [3H]Gpp(NH)p. In the presence of both PGE1 and epinephrine, more [3H]Gpp(NH)p is released than when either hormone is present alone; at low GTP concentrations, the effects were virtually additive. In the same membrane preparations in which PGE1 stimulates and epinephrine inhibits adenylate cyclase activity, both hormones individually and in combination were found to stimulate the release of [3H]Gpp(NH)p. Low concentrations of Mn2+, previously found to preferentially uncouple hormonal inhibition of platelet adenylate cyclase, were found to preferentially attenuate epinephrine-induced [3H]Gpp(NH)p release, whereas PGE1-stimulated nucleotide release was inhibited only at relatively higher Mn2+ concentrations. These data suggest that hormonal inhibition and stimulation of adenylate cyclase are mediated by analogous regulatory mechanisms at distinct guanine nucleotide binding sites.