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Inhibition of oxytocin receptor function by direct binding of progesterone

Eric Grazzini, Gilles Guillon, Bernard Mouillac and Hans H. Zingg ()
Additional contact information
Eric Grazzini: Laboratory of Molecular Endocrinology, Royal Victoria Hospital Research Institute, McGill University
Gilles Guillon: Unité INSERM U469, Centre de PharmacologieEndocrinologie
Bernard Mouillac: Unité INSERM U469, Centre de PharmacologieEndocrinologie
Hans H. Zingg: Laboratory of Molecular Endocrinology, Royal Victoria Hospital Research Institute, McGill University

Nature, 1998, vol. 392, issue 6675, 509-512

Abstract: Abstract The steroid hormone progesterone (P4) is essential for establishing and maintaining pregnancy in mammals1,2,3. One of its functions includes maintenance of uterine quiescence by decreasing uterine sensitivity to the uterotonic peptide hormone oxytocin3,4,5. Although it is generally held that steroid hormones such as P4 act at a genomic level by binding to nuclear receptors and modulating the expression of specific target genes6, we show here that the effect of P4 on uterine sensitivity to oxytocin involves direct, non-genomic action of P4 on the uterine oxytocin receptor (OTR), a member of the G-protein-coupled receptor family. P4 inhibits oxytocin binding to OTR-containing membranes in vitro, binds with high affinity to recombinant rat OTR expressed in CHO cells, and suppresses oxytocin-induced inositol phosphate production and calcium mobilization. These effects are highly steroid- and receptor-specific, because binding and signalling functions of the closely related human OTR are not affected by P4 itself but by the P4 metabolite 5β-dihydroprogesterone. Our findings provide the first evidence for a direct interaction between a steroid hormone and a G-protein-coupled receptor and define a new level of crosstalk between the peptide- and steroid-hormone signalling pathways.

Date: 1998
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DOI: 10.1038/33176

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