Placental Labyrinth Formation in Mice Requires Endothelial FLRT2/UNC5B Signaling

Overview

Journal Development

Specialty Biology

Date 2017 Jun 4

PMID 28576770

Citations 18

Authors

Ikue Tai-Nagara

Yusuke Yoshikawa

Naoko Numata

Tomofumi Ando

Keisuke Okabe

Yuki Sugiura

Masaki Ieda

Nobuyuki Takakura

Osamu Nakagawa

Bin Zhou

Koji Okabayashi

Makoto Suematsu

Yuko Kitagawa

Martin Bastmeyer

Kohji Sato

Rudiger Klein

Sutip Navankasattusas

Dean Y Li

Satoru Yamagishi

Yoshiaki Kubota

Affiliations

Soon will be listed here.

Abstract

The placental labyrinth is the interface for gas and nutrient exchange between the embryo and the mother; hence its proper development is essential for embryogenesis. However, the molecular mechanism underlying development of the placental labyrinth, particularly in terms of its endothelial organization, is not well understood. Here, we determined that fibronectin leucine-rich transmembrane protein 2 (FLRT2), a repulsive ligand of the UNC5 receptor family for neurons, is unexpectedly expressed in endothelial cells specifically in the placental labyrinth. Mice lacking FLRT2 in endothelial cells exhibited embryonic lethality at mid-gestation, with systemic congestion and hypoxia. Although they lacked apparent deformities in the embryonic vasculature and heart, the placental labyrinths of these embryos exhibited aberrant alignment of endothelial cells, which disturbed the feto-maternal circulation. Interestingly, this vascular deformity was related to endothelial repulsion through binding to the UNC5B receptor. Our results suggest that the proper organization of the placental labyrinth depends on coordinated inter-endothelial repulsion, which prevents uncontrolled layering of the endothelium.

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