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Hyaluronan control of the primary vascular barrier during early mouse pregnancy is mediated by uterine NK cells
Ron Hadas, … , Nava Dekel, Michal Neeman
Ron Hadas, … , Nava Dekel, Michal Neeman
Published November 19, 2020
Citation Information: JCI Insight. 2020;5(22):e135775. https://doi.org/10.1172/jci.insight.135775.
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Research Article Angiogenesis Reproductive biology

Hyaluronan control of the primary vascular barrier during early mouse pregnancy is mediated by uterine NK cells

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Abstract

Successful implantation is associated with a unique spatial pattern of vascular remodeling, characterized by profound peripheral neovascularization surrounding a periembryo avascular niche. We hypothesized that hyaluronan controls the formation of this distinctive vascular pattern encompassing the embryo. This hypothesis was evaluated by genetic modification of hyaluronan metabolism, specifically targeted to embryonic trophoblast cells. The outcome of altered hyaluronan deposition on uterine vascular remodeling and postimplantation development were analyzed by MRI, detailed histological examinations, and RNA sequencing of uterine NK cells. Our experiments revealed that disruption of hyaluronan synthesis, as well as its increased cleavage at the embryonic niche, impaired implantation by induction of decidual vascular permeability, defective vascular sinus folds formation, breach of the maternal-embryo barrier, elevated MMP-9 expression, and interrupted uterine NK cell recruitment and function. Conversely, enhanced deposition of hyaluronan resulted in the expansion of the maternal-embryo barrier and increased diffusion distance, leading to compromised implantation. The deposition of hyaluronan at the embryonic niche is regulated by progesterone-progesterone receptor signaling. These results demonstrate a pivotal role for hyaluronan in successful pregnancy by fine-tuning the periembryo avascular niche and maternal vascular morphogenesis.

Authors

Ron Hadas, Eran Gershon, Aviad Cohen, Ofir Atrakchi, Shlomi Lazar, Ofra Golani, Bareket Dassa, Michal Elbaz, Gadi Cohen, Raya Eilam, Nava Dekel, Michal Neeman

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Figure 3

Pharmacological blockade of the progesterone receptor after attachment.

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Pharmacological blockade of the progesterone receptor after attachment.
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Female ICR mice were mated with ICR males and administered with RU-486 at E4.5. Their uterine horns were harvested at E5.5 (n = 3 dams). (A) Representative images of VEGF-A staining in E5.5 decidua. (B) Smaller decidua and abnormal embryonic morphology, detected by H&E staining. (C) Comparison of cytokeratin-7–expressing trophoblast cells and their distribution; white arrows indicate embryos. (D) Representative images of decreased Hyal-2 decidual distribution. (E) Western blot analysis of Hyal-2 following RU-486 treatment (n = 4 dams; pools of 3 decidua). (F) Representative images of Hyal-1 staining in E5.5 decidua.

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