ITA
ENG

PARTICIPATION OF OPIOID AND SEROTONINERGIC SYSTEMS IN PROLACTIN SECRETION INDUCED BY HYPOTHALAMIC ACTION OF ESTRADIOL

Authors

CARON RW DEIS RP

Citation

Rw. Caron et Rp. Deis, PARTICIPATION OF OPIOID AND SEROTONINERGIC SYSTEMS IN PROLACTIN SECRETION INDUCED BY HYPOTHALAMIC ACTION OF ESTRADIOL, Neuroendocrinology, 64(2), 1996, pp. 124-130

Citations number

Categorie Soggetti

Neurosciences,"Endocrynology & Metabolism

Journal title

Neuroendocrinology → ACNP

ISSN journal

00283835

Volume

Issue

Year of publication

1996

Pages

124 - 130

Database

ISI

SICI code

0028-3835(1996)64:2<124:POOASS>2.0.ZU;2-P

Abstract

The aim of the present study was to determine the central effect of es tradiol (E(2)) on the pattern of secretion of prolactin (PRL) in virgi n rats and the participation of opioid and serotoninergic systems in t he regulation of this secretion. Bilateral cannulae containing E(2) (g roup E) or cholesterol (group C) were implanted in the arcuate nucleus on the day of estrus (day 0). Blood samples were obtained at 09.00, 1 4.00, or 18.00 h on days 1, 3, 6, or 9, All rats were blood sampled on ce, In group E, the PRL levels at 09.00 h on days 1 and 3 were similar to those from group C. However, higher values were obtained at 14.00 and 18.00 h, thus showing a diurnal rhythm with low levels in the morn ing and high values during the afternoon. No rhythm in PRL secretion w as observed on days 6 and 9 in group E in which serum PRL was similarl y increased with respect to group C al all times. The progesterone (P) levels paralleled PRL concentration, being significantly higher in gr oup E at 18.00 h on day 1, at 14.00 and 18.00 h on day 3, and at all t hree times on days 6 and 9; the P measurements were consistent with lu teotropic actions of PRL. Naloxone (NAL; 2 mg/kg i.p.) was injected at 17.30 h on days 3, 6, or 17, and 30 min later the animals were blood sampled. p-Chlorophenylalanine (pCPA: 200 mg/kg s.c.) was administered at 07.00 h on days 3, 5, or 16, and blood samples were taken 35 h lat er. Control E rats were injected with vehicle and blood sampled at 18. 00 h on days 3, 6, or 17. The PRL increase induced by E(2) at 18.00 h on days 3 and 6 was not modified by pretreatment with NAL or pCPA. Ser um P was significantly reduced after pCPA administration on days 3 and 6 and after NAL only on day 6. The increase in PRL at 18.00 h on day 17 induced by E(2) was dramatically enhanced by NAL or pCPA, while the se treatments did not significantly modify serum P levels. Our results indicate an inhibitory influence from both opioid and serotoninergic systems on PRL secretion induced by the long-term application of E(2) in the arcuate nucleus.