Your search keyword '"Rapetti D"' showing total 3 results

1. Evidence for a Role of the GHS-R1a Receptors in Ghrelin Inhibition of Gastric Acid Secretion in the Rat

Author

Sibilia, V., Muccioli, G., Deghenghi, R., Pagani, F., De Luca, V., Rapetti, D., Locatelli, V., and Netti, C.

Published

2006

2. Evidence for a Role of the GHS‐R1a Receptors in Ghrelin Inhibition of Gastric Acid Secretion in the Rat

Author

Sibilia, V., primary, Muccioli, G., additional, Deghenghi, R., additional, Pagani, F., additional, De Luca, V., additional, Rapetti, D., additional, Locatelli, V., additional, and Netti, C., additional

Published

2005

3. Evidence for a Role of the GHS-R1a Receptors in Ghrelin Inhibition of Gastric Acid Secretion in the Rat.

Author

Sibilia, V., Muccioli, G., Deghenghi, R., Pagani, F., De Luca, V., Rapetti, D., Locatelli, V., and Netti, C.

Subjects

GHRELIN, GASTROINTESTINAL hormones, GASTRIC acid, BIOLOGICAL transport, SOMATOSTATIN, SECRETION, NEUROPEPTIDES

Abstract

Ghrelin, the endogenous ligand of the GH secretagogue receptor (GHS-R) has been previously shown to inhibit gastric acid secretion in pylorus-ligated rats. Two isoforms of GHS-R have been identified: GHS-R1a and GHS-R1b. The present study aimed: (i) to characterise the type of GHS-R involved in the central gastric inhibitory activity of ghrelin by using des-octanoyl ghrelin, and synthetic GHS-R1a agonist (EP1572) and antagonist (D-Lys3-GHRP-6) and (ii) to investigate the relationship between ghrelin and cortistatin (CST) in the control of gastric acid secretion by using the natural neuropeptide CST-14 and the synthetic octapeptide CST-8. The specific interactions of all the compounds with GHS-R1a were determined by comparing their ability to displace labelled ghrelin or somatostatin from its receptors on rat hypothalamic membranes or on rat cardiomyocyte, respectively. Intracerebroventricular administration of 0.01 and 1 nmol/rat des-octanoyl ghrelin did not affect gastric acid secretion in pylorus-ligated rats, whereas EP1572 either i.c.v. (0.01–1 nmol/rat) or i.p. (10 and 20 nmol/kg) inhibited acid gastric secretion. Preteatment with D-Lys3GHRP-6 (3 nmol/rat, i.c.v.) was able to remove the inhibitory action of ghrelin (0.01 nmol/rat, i.c.v.) on gastric acid volume and acid output, thus indicating that the type 1a GHS-R likely mediates the gastric inhibitory action of ghrelin. This is supported by binding data showing that D-Lys3GHRP-6, but not des-octanoyl ghrelin, binds to hypothalamic GHS-R. CST-14 (1 nmol/rat, i.c.v.) did not affect either basal or ghrelin inhibition of gastric acid secretion. CST-8 (1 nmol/rat, i.c.v.) was able to counteract the gastric ghrelin response. The observation that CST-14 binds both GHR-S and somatostatin receptors, whereas CST-8 specifically displaces only ghrelin binding, indicates that CST-8 behaves as a GHS-R1a antagonist. [ABSTRACT FROM AUTHOR]

Published

2006