Proadrenomedullin N-Terminal 20 Peptide (PAMP), Acting Through PAMP(12–20)-Sensitive Receptors, Inhibits Ca2+-Dependent, Agonist-Stimulated Secretion of Human Adrenal Glands

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Hypertension. 1999;33:1185-1189

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(Hypertension. 1999;33:1185-1189.)
© 1999 American Heart Association, Inc.

Scientific Contributions

Proadrenomedullin N-Terminal 20 Peptide (PAMP), Acting Through PAMP(12–20)-Sensitive Receptors, Inhibits Ca²⁺-Dependent, Agonist-Stimulated Secretion of Human Adrenal Glands

Anna S. Belloni; Gian Paolo Rossi; Paola G. Andreis; Francesco Aragona; Hunter C. Champion; Philip J. Kadowitz; William A. Murphy; David H. Coy; Gastone G. Nussdorfer

From the Departments of Anatomy (A.S.B., P.G.A., G.G.N.), Clinical and Experimental Medicine (G.P.R.), and Urology (F.A.), School of Medicine, University of Padua, Padua, Italy; and the Departments of Pharmacology (H.C.C., P.J.K.) and Medicine (W.A.M., D.H.C.), School of Medicine, Tulane University, New Orleans, La.

Correspondence to Professor Gastone G. Nussdorfer, Department of Anatomy, Via Gabelli 65, I-35121 Padova, Italy. E-mail ggnanat{at}ipdunidx.unipd.it

Abstract—Proadrenomedullin N-terminal 20 peptide (PAMP)is a 20–amino acid hypotensive peptide expressed in theadrenal medulla. We investigated the localization and functionof PAMP receptors in the human adrenal gland. Autoradiographyshowed the presence of [¹²⁵I]PAMP-binding sites in both zonaglomerulosa and adrenal medulla that were displaced by coldPAMP and PAMP(12–20) but not by other preproadrenomedullin-derivedpeptides. PAMP, but not PAMP(12–20), counteracted, in aconcentration dependent manner, both aldosterone response ofzona glomerulosa cells and catecholamine response of adrenalmedulla cells to BAYK-8644, the selective agonist of voltage-activated Ca²⁺channels, as well as to K⁺ and angiotensin II. PAMP(12–20)partially reversed this antisecretagogue effect of PAMP. Collectively,these findings suggest (1) that PAMP inhibits Ca²⁺-dependent,agonist-stimulated aldosterone and catecholamine secretion,acting via specific receptors and through a mechanism involvingthe impairment of Ca²⁺ influx; and (2) that PAMP(12–20)acts as a weak antagonist of PAMP receptors, thereby suggestingthat both C- and N-terminal sequences of the PAMP molecule arerequired for this peptide to exert its antisecretagogue actionon the human adrenal gland.

Key Words: PAMP • adrenal glands • aldosterone • catecholamines

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