In this study, we investigated the effects of ablation of uterine Forkhead Box A2 () on gene expression of fetal brain relative to placenta. Using a conditional knockout mouse model for uterine , here we show that the lack of uterine elicits a sexually-conflicting transcriptional response in the fetal brain relative to placenta. The ablation of in the uterus altered expression of genes related to growth, nutrient sensing, aging, longevity and angiogenesis among others. In the wildtype mice, these genes were expressed higher in the fetal brain and placenta of males compared to females. However, in mice lacking uterine , the same genes showed the opposite pattern i.e., higher expression in the fetal brain and placenta of females compared to males. Based on the known marker genes of mice placenta and fetal brain cells, we further predicted that the genes exhibiting the sexually conflicting expression were associated with vascular endothelial cells. Overall, our study suggests that uterine plays a role in the regulation of the brain-placental axis by influencing the fetoplacental vascular changes during pregnancy.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8468108PMC
http://dx.doi.org/10.3390/ijms22189693DOI Listing

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