The effect may reveal an underlying factor in what has been found to be an increased risk of preterm birth among those who use antidepressants during pregnancy and possible therapeutic targets to reduce that risk.
As many as 13% of pregnant people will use antidepressants during their pregnancy, according to previous research.
Yet a common type of antidepressant, known as a serotonin reuptake inhibitor (SRI), can have various adverse effects on fetuses and pregnancies. The strongest evidence points to increased risks of a pregnant person’s water breaking too early and subsequent preterm delivery.
Pregnant people with psychiatric illnesses, therefore, face the tough decision of whether to stop treatment.
“It’s hard to suddenly take a pregnant person off of a medication they need,” says Vikki Abrahams, professor of obstetrics, gynecology, and reproductive sciences at Yale University School of Medicine. “If we can identify a way to prevent an adverse pregnancy outcome, we could reduce the risk of SRI treatment.”
Abrahams is co-senior author of the study in the Journal of Reproductive Immunology, along with Kimberly Yonkers at the University of Massachusetts Chan Medical School.
Water-breaking refers to when the amniotic sac ruptures, and it’s a sign that labor has started or soon will. When that happens before a pregnancy has reached term, it’s known as preterm premature rupture of membranes.
“When it happens too early, it triggers preterm labor, and we know that prematurity is really detrimental to the baby and that it can have long-term health consequences for the child later in life,” says Abrahams.
Inflammation in the fetal membranes—the amniotic sac that encloses the fetus and amniotic fluid—is thought to be one cause of preterm premature rupture of membranes. To see if inflammation plays a role in the adverse pregnancy effects of SRIs, Abrahams and her colleagues analyzed the effects of Prozac, also known as fluoxetine, on fetal membranes.
The researchers used samples of human fetal membrane tissue donated to the Yale University Reproductive Sciences Biobank and collected from uncomplicated pregnancies delivered via caesarean section. They exposed some tissue samples to Prozac and compared them to samples not exposed to the drug.
They found that Prozac increased the activity levels of a molecule called p38-MAPK that mediates inflammation. That molecule, in turn, caused an increase of interleukin 6, a small protein called a cytokine that promotes inflammation.
The researchers then analyzed fetal membrane samples collected from people who had used Prozac during pregnancy, compared them to samples from people who did not use antidepressants, and found they too had elevated levels of active p38-MAPK.
The findings reveal potential targets for treatment.
“There’s evidence in other disease models that targeting inflammatory cytokines may be an option,” says Abrahams. “People with lupus, for example, are at higher risk for adverse pregnancy outcomes and there are clinical trials under way in which these patients are being treated with antibodies that target a particular cytokine. So here, anti-interleukin 6 antibodies, for instance, could be worth investing.”
Ultimately, the study reveals a signaling pathway to investigate further, which could yield even better targets for treatment, she adds.
Going forward, Abrahams is interested in uncovering how SRIs like Prozac act on the fetal membranes to elevate p38-MAPK, how other SRIs affect fetal membranes, and whether other types of antidepressants have similar effects.
For now, though, knowing that SRIs can cause inflammation in fetal membranes will help with decision-making and clinical management, says Abrahams.
“It arms the physician and the patient with more information,” she says. “And that can help them make more informed choices.”
Source: Mallory Locklear for Yale University
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