Vasopressin receptors influencing the secretion of ACTH by the rat adenohypophysis

Abstract

The effects of selective agonists and antagonists of type 1 (V₁) and type 2 (V₂) vasopressin receptors on the secretion of ACTH in vitro by segments of adenohypophysial tissue and in vivo in rats pretreated with pentobarbitone and chlorpromazine were studied in the presence and absence of the 41 amino acid-containing peptide, corticotrophin-releasing factor-41 (CRF-41). The non-selective vasopressin receptor agonist, arginine vasopressin (AVP) and the V₁-receptor agonist, felypressin caused dose-related increases in ACTH release in vivo and in vitro but the V₂-receptor agonist, desmopressin was only weakly active in this respect. Their actions in vitro were antagonized competitively by the V₁-receptor antagonist, d(C₂H₅)₂-AVP, but were unaffected by the V₂-receptor antagonist, d(CH₂)₅-d-Iso²-Thr⁴-AVP. Arginine vasopressin, felypressin and desmopressins in concentrations considerably lower than those necessary to elicit directly the release of ACTH, potentiated, in a dose-related manner, the activity of CRF-41 in vitro. The potentiating effects were not antagonized by the V₂-receptor antagonist or by low concentrations of the V₁ -receptor antagonist. At a higher concentration, the V₁-receptor antagonist reduced, but did not abolish, the potentiating effects of AVP and its analogues. However, at this concentration, it also exhibited weak intrinsic activity and, like the agonists, potentiated the response to CRF-41. The results suggest that the direct effect of AVP on ACTH release is mediated by V₁-like receptors. The vasopressin receptors involved in the potentiation of CRF-41 activity appear to be different. J. Endocr. (1987) 113, 389–396