The human fetal membranes: a target tissue for relaxin

The purpose of this study was to adduce further evidence for a paracrine role for human decidual relaxin (Rlx) in the remodelling of collagen in the fetal membranes in the peripartal period. The binding of [125I]porcine Rlx to membrane-enriched fractions from fetal membranes as well as from disperse...

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Published inThe journal of clinical endocrinology and metabolism Vol. 62; no. 3; p. 513
Main Authors Koay, E S, Bryant-Greenwood, G D, Yamamoto, S Y, Greenwood, F C
Format Journal Article
LanguageEnglish
Published United States 01.03.1986
Subjects
Amnion - metabolism
Amniotic Fluid - metabolism
Chorion - metabolism
Extraembryonic Membranes - metabolism
Female
Gestational Age
Glucuronidase - metabolism
Humans
In Vitro Techniques
Microbial Collagenase - metabolism
Placenta - metabolism
Plasminogen Activators - metabolism
Pregnancy
Receptors, G-Protein-Coupled
Receptors, Neurotransmitter - metabolism
Receptors, Peptide
Relaxin - metabolism
Relaxin - physiology
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Summary:The purpose of this study was to adduce further evidence for a paracrine role for human decidual relaxin (Rlx) in the remodelling of collagen in the fetal membranes in the peripartal period. The binding of [125I]porcine Rlx to membrane-enriched fractions from fetal membranes as well as from dispersed cells from the fetal membranes was used to demonstrate the presence of specific Rlx receptors. Rlx added in vitro to cultured amnion/chorion cells increased the release of plasminogen activator and collagenase into the medium. Rlx had no effect on the release of beta-glucuronidase. An in vivo correlate of these in vitro results was obtained, the detection of plasminogen activator and collagenase in amniotic fluids. The active fraction of collagenase was increased in amniotic fluids collected after spontaneous rupture of the membranes. PRL, hCG, estrogen, and progesterone added in equimolar amounts to cultured amnion/chorion cells from elective cesarean sections and normal term deliveries also effected the release of plasminogen activator and collagenase. The greatest effects were found in cells from cesarean section tissue, in terms of the stimulation of plasminogen activator release by Rlx and PRL and of collagenase release by prostaglandin F2 alpha and, to a lesser extent, by Rlx, PRL, and hCG. We conclude that human fetal membranes are targets for a number of hormones, including the decidual paracrine hormones Rlx, PRL, and prostaglandin F2 alpha as well as estrogen, progesterone, and hCG. These hormones act to release or inhibit the enzymes involved in collagen breakdown before rupture of the fetal membranes.
ISSN:0021-972X
DOI:10.1210/jcem-62-3-513