Sexually Dimorphic Crosstalk at the Maternal-Fetal Interface

母胎界面的性别二态串扰

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作者:Tianyanxin Sun, Tania L Gonzalez, Nan Deng, Rosemarie DiPentino, Ekaterina L Clark, Bora Lee, Jie Tang, Yizhou Wang, Barry R Stripp, Changfu Yao, Hsian-Rong Tseng, S Ananth Karumanchi, Alexander F Koeppel, Stephen D Turner, Charles R Farber, Stephen S Rich, Erica T Wang, John Williams, Margareta D P

Conclusions

Maternal-fetal crosstalk exhibits sexual dimorphism during placentation early in gestation.

Objective

Investigate the impact of fetal sex on maternal-fetal crosstalk. Design: Receptors/ligands at the maternal-fetal surface were identified from sexually dimorphic genes between fetal sexes in the first trimester placenta and defined in each cell type using single-cell RNA-Sequencing (scRNA-Seq). Setting: Academic institution. Samples: Late first trimester (~10-13 weeks) placenta (fetal) and decidua (maternal) from uncomplicated ongoing pregnancies. Main outcome measures: Transcriptomic profiling at tissue and single-cell level; immunohistochemistry of select proteins.

Results

We identified 91 sexually dimorphic receptor-ligand pairs across the maternal-fetal interface. We examined fetal sex differences in 5 major cell types (trophoblasts, stromal cells, Hofbauer cells, antigen-presenting cells, and endothelial cells). Ligands from the CC family chemokine ligand (CCL) family were most highly representative in females, with their receptors present on the maternal surface. Sexually dimorphic trophoblast transcripts, Mucin-15 (MUC15) and notum, palmitoleoyl-protein carboxylesterase (NOTUM) were also most highly expressed in syncytiotrophoblasts and extra-villous trophoblasts respectively. Gene Ontology (GO) analysis using sexually dimorphic genes in individual cell types identified cytokine mediated signaling pathways to be most representative in female trophoblasts. Upstream analysis demonstrated TGFB1 and estradiol to affect all cell types, but dihydrotestosterone, produced by the male fetus, was an upstream regulator most significant for the trophoblast population. Conclusions: Maternal-fetal crosstalk exhibits sexual dimorphism during placentation early in gestation.

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