Abstract

Maternal spiral arteries and newly formed decidual capillaries support embryonic development prior to placentation. Previous studies demonstrated that Notch signaling is active in endothelial cells of both decidual capillaries and spiral arteries, however the role of Notch signaling in physiologic decidual angiogenesis and maintenance of the decidual vasculature in early mouse pregnancy has not yet been fully elucidated. We used the Cdh5-CreERT2; Jagged1(Jag1)flox/flox (Jag1∆EC) mouse model to delete Notch ligand, Jag1, in maternal endothelial cells during post-implantation, pre-placentation mouse pregnancy. Loss of endothelial Jag1 leads to increased expression of Notch effectors, Hey2 and Nrarp, and increased endothelial Notch signaling activity in areas of the decidua with remodeling angiogenesis. This correlated with an increase in Dll4 expression in capillary endothelial cells, but not spiral artery endothelial cells. Consistent with increased Dll4/Notch signaling, we observed decreased VEGFR2 expression and endothelial cell proliferation in angiogenic decidual capillaries. Despite aberrant Dll4 expression and Notch activation in Jag1∆EC mutants, pregnancies were maintained and the decidual vasculature was not altered up to embryonic day 7.5. Thus, Jag1 functions in the newly formed decidual capillaries as an antagonist of endothelial Dll4/Notch signaling during angiogenesis, but Jag1 signaling is not necessary for early uterine angiogenesis.

Highlights

  • During early pregnancy, from embryo implantation to placentation, formation of new capillaries and physiologic remodeling of uterine spiral arteries (SpAs), which are distal branches of the maternal uterine arteries, are essential for normal embryonic growth and development [1,2,3]

  • We focused on the role the endothelial Jag1 in decidual vasculature in the

  • We focused on the role the endothelial Jag1 in decidual vasculature in the postpost-implantation, pre-placentation mouse uterus

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Summary

Introduction

From embryo implantation to placentation, formation of new capillaries and physiologic remodeling of uterine spiral arteries (SpAs), which are distal branches of the maternal uterine arteries, are essential for normal embryonic growth and development [1,2,3].

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