4.1 Article

Prenatal antidepressant exposure and sex differences in neonatal corpus callosum microstructure

期刊

DEVELOPMENTAL PSYCHOBIOLOGY
卷 63, 期 6, 页码 -

出版社

WILEY
DOI: 10.1002/dev.22125

关键词

diffusion tensor imaging; discriminant analysis; neonatal brain; selective serotonin reuptake inhibitors; sex differences; white matter

资金

  1. BC Children's Hospital Research Institute
  2. Canadian Institutes of Health Research [MOP-119302]
  3. Brain Canada-Kids Brain Health Fellowship in Developmental Neuroscience, through the Canadian Brain Research Fund
  4. Health Canada (KSJC)
  5. Doctoral Fellowship from the Faculty of Graduate and Postdoctoral Studies at the University of British Columbia (KSJC)
  6. Bloorview Children's Hospital Chair in Pediatric Neuroscience (SPM)

向作者/读者索取更多资源

The study suggests that prenatal exposure to selective serotonin reuptake inhibitors (SSRIs) may have sex-specific effects on the microstructure of the neonatal corpus callosum (CC), indicating a localized developmental sensitivity to SSRI exposure in early stages.
Prenatal exposure to selective serotonin reuptake inhibitor (SSRI) antidepressants may influence white matter (WM) development, as previous studies report widespread microstructural alterations and reduced interhemispheric connectivity in SSRI-exposed infants. In rodents, perinatal SSRIs had sex-specific disruptions in corpus callosum (CC) axon architecture and connectivity; yet it is unknown whether SSRI-related brain outcomes in humans are sex specific. In this study, the neonate CC was selected as a region-of-interest to investigate whether prenatal SSRI exposure has sex-specific effects on early WM microstructure. On postnatal day 7, diffusion tensor imaging was used to assess WM microstructure in SSRI-exposed (n = 24; 12 male) and nonexposed (n = 48; 28 male) term-born neonates. Fractional anisotropy was extracted from CC voxels and a multivariate discriminant analysis was used to identify latent patterns differing between neonates grouped by SSRI-exposure and sex. Analysis revealed localized variations in CC fractional anisotropy that significantly discriminated neonate groups and correctly predicted group membership with an 82% accuracy. Such effects were identified across three dimensions, representing sex differences in SSRI-exposed neonates (genu, splenium), SSRI-related effects independent of sex (genu-to-rostral body), and sex differences in nonexposed neonates (isthmus-splenium, posterior midbody). Our findings suggest that CC microstructure may have a sex-specific, localized, developmental sensitivity to prenatal SSRI exposure.

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