Abstract
Arginine-vasopressin (AVP) seems to be involved in the histamine (HA)- and stress-induced release of ACTH and β-endorphin (β-END). We studied the effect of selective AVP V1- or V2-receptor blockade on the ACTH and β-END response to HA or restraint stress in conscious male rats. HA (270 nmol) administered intracerebroventricularly or 5 min of restraint stress caused a 3-to 7-fold increase in the plasma levels of ACTH and β-END immunoreactivity (β-ENDir). Pretreatment of the animals with the nonselective V1+2-receptor antagonist [l-Pmp-2-Z)-Phe-4-Ile-8-Arg]vasopressin, which was administered intravenously in a low (23 nmol) or a high dose (90 nmol) inhibited the HA-or restraint stress-induced secretion of ACTH and β-ENDir 60 and 25-70%, respectively. Pretreatment with equipotent doses of the selective V1-receptor antagonist [l-(p-tBu)Pmp-2-Tyr(0-Me)-8-D-Arg]vasopressin (25 nmol) and/or the selective V2-receptor antagonist [l-Pmp-2-D-IIe-4-Ile-8-Arg]vasopres-sin (7.0 nmol) attenuated the response of ACTH and β-ENDir to HA or restraint stress by 60-80 and 40-60%, respectively. In general, these doses of antagonists had no effect on basal hormone levels. We conclude that AVP takes part in the mediation of HA- and restraint stress-induced ACTH and β-END secretion. This effect seems to be mediated via both AVP V1 and V2-receptors or a less selective receptor with ligand specificity for both V1- and V2-receptor antagonists.
Originalsprog | Engelsk |
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Tidsskrift | Neuroendocrinology |
Vol/bind | 57 |
Udgave nummer | 3 |
Sider (fra-til) | 503-509 |
Antal sider | 7 |
ISSN | 0028-3835 |
DOI | |
Status | Udgivet - 1993 |