Molecular basis of bone morphogenetic protein-4 inhibitory action on progesterone secretion by ovine granulosa cells

doi:10.1677/jme.1.01545

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Molecular basis of bone morphogenetic protein-4 inhibitory action on progesterone secretion by ovine granulosa cells

A Pierre, C Pisselet, J Dupont, B Mandon-Pépin¹, D Monniaux, P Monget and S Fabre

Physiologie de la Reproduction et des Comportements, UMR 6175 INRA-CNRS-Université de Tours, Haras Nationaux, 37380 Nouzilly, France
¹ Biologie du Développement et de la Reproduction, UMR 1198 INRA-ENVA, 78350 Jouy en Josas, France

(Requests for offprints should be addressed to S Fabre; Email: sfabre{at}tours.inra.fr)

We have recently reported that bone morphogenetic protein-4(BMP-4) can inhibit progesterone production by ovine granulosacells (GCs). Here, we have investigated the underlying mechanismsof this effect in basal as well as in FSH-induced conditions.We have confirmed that treatment with BMP-4 decreased basalGC progesterone secretion and totally abolished FSH-stimulatingaction. This inhibitory action was associated with a decreasein the expression of cAMP-regulated genes, steroidogenic acuteregulatory protein (StAR) and P450 side-chain cleavage (P450scc) at mRNA and protein levels. However, BMP-4 did not alterbasal cAMP production by GCs. In contrast, BMP-4 decreased byhalf the FSH-induced cAMP production and strongly inhibitedcAMP-induced progesterone production. Thus, the inhibitory effectof BMP-4 was exerted both upstream and downstream of cAMP signalling.We next examined the downstream effect, focusing on cAMP-dependenttranscription factors, steroidogenic factor-1 (SF-1) and CREB,through the BMP factor signalling intermediary, Smad1. As expected,BMP-4 induced phosphorylation and transcriptional activity ofSmad1 in ovine GCs. BMP-4-activated Smad1 did not affect CREBactivity but inhibited the transcriptional activity of SF-1on the canonical SF-1 responsive element. Interestingly, thistranscriptional inhibitory mechanism occurred on transfectedStAR and P450 scc promoter. Based on these results, we proposethat SF-1 is a key target in the inhibitory mechanism exertedby BMP-4 on progesterone synthesis by ovine GCs in culture.Because SF-1 plays an essential role in the differentiationof GCs, our findings could have new implications in understandingthe role of BMP family members in the control of ovarian folliculogenesis.

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