Pregnancy Clinical Trial
Official title:
Inflammatory Signature of Chorionic Cells as Markers of Premature Labor
The purpose of this study is to identify molecules produced specifically by the cells from the chorionic membranes of the materno-fetal interface ("the water bag") sign for the activation of preterm labor.
· Background
During human gestation, fetal membranes (the "water bag") encompass the amnion, facing the
amniotic cavity, and the chorion, lining the maternal decidua and comprising trophoblast
cells. Membranes usually remain intact until their spontaneous rupture, close to the first
stage of labor at term. Often seen as a simple inert shell, with a role of "airbag" for the
developing fetus, the membranes provide yet a large surface of interaction between maternal
and fetal tissues and function as a transient endocrine organ with immune properties. Indeed
human parturition is tightly correlated with hormonal changes at the maternal-fetal
interface during pregnancy, that may control cell interactions and chorio-decidua
remodeling, the amnion remaining usually intact until the final break. Precocious remodeling
may lead to a premature onset of labor, associated or not with premature rupture of membrane
whether the cause is infectious or not. A better understanding of this membrane remodeling
may thus offer new avenues to define biomarkers of preterm labor.
Hereof, the fact that the mother-to-be accepts and keeps the fetus for months within her
womb has long being seen as an enigma, since the fetus is a semi-allograft, half of his
genome being of paternal, thus of foreign, origin. This apparent paradox was deciphered by
the demonstration of the set-up of an immunotolerance at the site of implantation through
the education of maternal immune cells (Natural Killer and T cells) by the fetal
trophoblast. This immunotolerance is normally maintained throughout pregnancy, and some
recurrent spontaneous miscarriages have been shown to be due to the loss of this
immunotolerance, which activates the rejection of the semi-allograft.
In this regard, remodeled fetal membranes overlying the cervix may discharge signals that
could be detectable in cervicovaginal fluids and serve as biomarkers of the imminence of
delivery. Such information on delivery timing may be of great importance for an adequate
prediction that would change drastically the management of threatening preterm delivery.
· Current proposal The objective of this study is to characterize the fetal and maternal
cells in the chorio-decidua during the remodeling of the membranes using our
well-established cell model (Hervé et al. 2008, J Immunol).
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Observational Model: Cohort, Time Perspective: Prospective
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