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Prenatal Stress and Early-life Exposure to Fluoxetine Have Enduring Effects on Anxiety and Hippocampal BDNF Gene Expression in Adult Male Offspring

Overview
Journal Dev Psychobiol
Specialties Pediatrics
Psychiatry
Psychology
Date 2015 Nov 27
PMID 26608001
Citations 20
Authors
Fabien Boulle
Jodi L Pawluski
Judith R Homberg
Barbie Machiels
Yvet Kroeze
Neha Kumar
Harry W M Steinbusch
Gunter Kenis
Daniel L A van den Hove
Affiliations
Soon will be listed here.
Abstract

With the growing use of selective serotonin reuptake inhibitor medications (SSRIs) for the treatment of depression during the perinatal period, questions have been raised about the longterm impact of these medications on development. We aimed to investigate how developmental SSRI exposure may alter affect-related behaviors and associated molecular processes in offspring using a rodent model of maternal stress and depression. For this purpose, prenatally stressed or non-stressed male offspring were exposed to fluoxetine (5 mg/kg/day) or vehicle, via lactation, until weaning. Primary results show that postnatal fluoxetine exposure differentially altered anxiety-like behavior by increasing anxiety in non-stressed offspring and decreasing anxiety in prenatally stressed offspring. In the hippocampus, developmental fluoxetine exposure decreased BDNF IV and TrkB mRNA expression. Prenatal stress alone also decreased escape behaviors and decreased hippocampal BDNF IV mRNA expression. These data provide important evidence for the long-term programming effects of early-life exposure to SSRIs on brain and behavior.

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