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Use of SSRIs During Pregnancy May Cause Neurologic
Symptoms in Newborns
Laurie Barclay, MD
July 14, 2003 — Newborns of mothers receiving fluoxetine or
citalopram exhibited symptoms of central serotonin overstimulation
for about four days, according to the results of a prospective trial
published in the July issue of the Archives of General
Psychiatry. The investigators warn of potential neurologic
adverse effects from selective serotonin reuptake inhibitors (SSRIs)
used during late pregnancy.
"SSRIs have gained wide acceptance in the treatment of mental
disorders in pregnant women, but there seems to be an increased risk
for neonatal adaptation problems after exposure to SSRIs in late
pregnancy," write Kari Laine, MD, PhD, from the University of Turku
in Finland, and colleagues. They cite previous studies suggesting
that exposure to SSRIs during the third trimester may cause
irritability, constant crying, eating and sleeping difficulties, and
even seizures in newborns.
Between January 1, 1997, and August 31, 2000, Dr. Laine's group
enrolled 40 pregnant women, including 20 who were taking SSRIs
during pregnancy and breast-feeding and 20 who were not taking any
psychoactive medications. All infants had neurologic assessments
during the first four days of life and at two weeks and two months
of age after delivery, as well as brain ultrasound and magnetic
resonance imaging (MRI) 38 to 42 weeks after conception and at two
months of age.
During the first two months of life, blood pressure, heart rate,
and body temperature were similar in both groups. During the first
four days of life, the serotonergic symptom score reflecting tremor,
restlessness, and rigidity was four times higher in the SSRI group
than in the control group (P = .008). Serotonin-related
symptoms declined significantly in the SSRI group from the first
four days to two weeks, and there was no significant difference in
serotonergic symptom score between the two groups at two weeks.
Cord blood concentration of 5-hydroxyindoleacetic acid (5-HIAA)
was significantly lower in the SSRI group than in the control group
(P = .02). Umbilical vein 5-HIAA concentration was inversely
correlated with serotonergic symptom score in the SSRI group (r =
-0.66; P = .007) but not in the control group.
Because the symptoms resolved quickly while SSRI concentrations
were decreasing, the authors suggest that the symptoms are related
to central nervous system serotonergic overstimulation rather than
to SSRI withdrawal syndrome.
"We report increased risk for central nervous system serotonergic
adverse effects during the first days of life in newborns of mothers
taking the SSRIs citalopram or fluoxetine during the third trimester
of pregnancy," they write. "The clinical relevance of the present
results is awareness of the psychiatrists who prescribe SSRIs during
pregnancy and the pediatricians who treat the serotonin-related
neurologic symptoms of the newborns during the first days of life.
Although these effects seem to subside quickly, they may expose the
infants to more serious neonatal complications such as
convulsions."
The Turku University Hospital Research Fund supported this
study.
Arch Gen Psychiatry. 2003;60:720-726
Reviewed by Gary D. Vogin, MD
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Laurie
Barclay, MD Writer for Medscape Medical News Medscape Medical
News is edited by Deborah Flapan, assistant managing editor of
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Medscape Medical News 2003. © 2003 Medscape
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