| Literature DB >> 33942888 |
Kayleigh S J Campbell1,2, Lynne J Williams1, Bruce H Bjornson1,3, Ella Weik1, Ursula Brain1,3, Ruth E Grunau1,3, Steven P Miller4, Tim F Oberlander1,3.
Abstract
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.Entities:
Keywords: diffusion tensor imaging; discriminant analysis; neonatal brain; selective serotonin reuptake inhibitors; sex differences; white matter
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Year: 2021 PMID: 33942888 DOI: 10.1002/dev.22125
Source DB: PubMed Journal: Dev Psychobiol ISSN: 0012-1630 Impact factor: 3.038