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Placental endocrine function shapes cerebellar development and social behavior

Authors :
Jacob Ellegood
Sonia Sebaoui
Aaron Sathyanesan
Kazue Hashimoto-Torii
Vittorio Gallo
Anastas Popratiloff
Yuka Imamura
Helene Lacaille
Jason P. Lerch
Michael Schumacher
Jacquelyn Salzbank
Panagiotis Kratimenos
Jiaqi J. O’Reilly
Dana Bakalar
Claire Marie Vacher
Philippe Liere
Cheryl Clarkson-Paredes
Anna A. Penn
Toru Sasaki
Source :
Nature Neuroscience
Publication Year :
2021
Publisher :
Nature Publishing Group US, 2021.

Abstract

Compromised placental function or premature loss has been linked to diverse neurodevelopmental disorders. Here we show that placenta allopregnanolone (ALLO), a progesterone-derived GABA-A receptor (GABAAR) modulator, reduction alters neurodevelopment in a sex-linked manner. A new conditional mouse model, in which the gene encoding ALLO’s synthetic enzyme (akr1c14) is specifically deleted in trophoblasts, directly demonstrated that placental ALLO insufficiency led to cerebellar white matter abnormalities that correlated with autistic-like behavior only in male offspring. A single injection of ALLO or muscimol, a GABAAR agonist, during late gestation abolished these alterations. Comparison of male and female human preterm infant cerebellum also showed sex-linked myelination marker alteration, suggesting similarities between mouse placental ALLO insufficiency and human preterm brain development. This study reveals a new role for a placental hormone in shaping brain regions and behaviors in a sex-linked manner. Placental hormone replacement might offer novel therapeutic opportunities to prevent later neurobehavioral disorders.<br />Placental dysfunction has been implicated in abnormal neurodevelopment. Vacher et al. found that loss of a neuroactive hormone from the placenta alters brain development in a regional and sex-linked manner, resulting in autism-like behaviors in male offspring.

Details

Language :
English
ISSN :
15461726 and 10976256
Volume :
24
Issue :
10
Database :
OpenAIRE
Journal :
Nature Neuroscience
Accession number :
edsair.doi.dedup.....e872b45fcc44db8841f91f322d2cf3eb