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Title

Single-cell RNA sequencing identifies CXADR as a fate determinant of the placental exchange surface.

Authors

Angelova, Dafina M.; Tsolova, Aleksandra; Prater, Malwina; Ballasy, Noura; Bacon, Wendi; Hamilton, Russell S.; Blackwell, Danielle; Yu, Ziyi; Li, Xin; Liu, Xin; Hemberger, Myriam; Charnock-Jones, D. Stephen

Abstract

The placenta is the critical interface between mother and fetus, and consequently, placental dysfunction underlies many pregnancy complications. Placental formation requires an adequate expansion of trophoblast stem and progenitor cells followed by finely tuned lineage specification events. Here, using single-cell RNA sequencing of mouse trophoblast stem cells during the earliest phases of differentiation, we identify gatekeepers of the stem cell state, notably Nicol1, and uncover unsuspected trajectories of cell lineage diversification as well as regulators of lineage entry points. We show that junctional zone precursors and precursors of one of the two syncytial layers of the mouse placental labyrinth, the Syncytiotrophoblast-I lineage, initially share similar trajectories. Importantly, our functional analysis of one such lineage precursor marker, CXADR, demonstrates that this cell surface protein regulates the differentiation dynamics between the two syncytial layers of the mouse labyrinth, ensuring the correct establishment of the placental exchange surface. Deciphering the mechanisms underlying trophoblast lineage specification will inform our understanding of human pregnancy in health and disease. Placental formation requires an adequate expansion of trophoblast stem and progenitor cells followed by finely tuned lineage specification events. Here, using single-cell analysis of mouse trophoblast stem cells the authors identify Nicol1 as a gatekeeper of the stem cell state and show that CXADR regulates the differentiation dynamics between the two syncytial layers of the mouse placenta.

Subjects

CYTOLOGY; LIFE sciences; MEDICAL sciences; PREGNANCY complications; PROGENITOR cells; TROPHOBLAST

Publication

Nature Communications, 2025, Vol 16, p1

ISSN

2041-1723

Publication type

Academic Journal

DOI

10.1038/s41467-024-55597-w

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