Oxytocin Facilitates Female Sexual Maturation through a Glia-to-Neuron Signaling Pathway

Author:

Parent Anne-Simone1,Rasier Grégory1,Matagne Valérie2,Lomniczi Alejandro2,Lebrethon Marie-Christine1,Gérard Arlette1,Ojeda Sergio R.2,Bourguignon Jean-Pierre1

Affiliation:

1. Developmental Neuroendocrinology Unit (A.-S.P., G.R., M.-C.L., A.G., J.-P.B.), University of Liège, 4000 Liège, Belgium

2. Division of Neuroscience (V.M., A.L., S.R.O.), Oregon National Primate Research Center, Beaverton, Oregon 97006

Abstract

It has been earlier proposed that oxytocin could play a facilitatory role in the preovulatory LH surge in both rats and humans. We here provide evidence that oxytocin also facilitates sexual maturation in female rats. The administration of an oxytocin antagonist for 6 d to immature female rats decreased GnRH pulse frequency ex vivo and delayed the age at vaginal opening and first estrus. The in vitro reduction in GnRH pulse frequency required chronic blockade of oxytocin receptors, because it was not acutely observed after a single injection of the antagonist. Hypothalamic explants exposed to the antagonist in vitro showed a reduced GnRH pulse frequency and failed to respond to oxytocin with GnRH release. Prostaglandin E2 (PGE2) mimicked the stimulatory effect of oxytocin on GnRH pulse frequency, and inhibition of PG synthesis blocked the effect of oxytocin, suggesting that oxytocin accelerates pulsatile GnRH release via PGE2. The source of PGE2 appears to be astrocytes, because oxytocin stimulates PGE2 release from cultured hypothalamic astrocytes. Moreover, astrocytes express oxytocin receptors, whereas GnRH neurons do not. These results suggest that oxytocin facilitates female sexual development and that this effect is mediated by a mechanism involving glial production of PGE2.

Publisher

The Endocrine Society

Subject

Endocrinology

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