What question did this study set out to answer?

The research aims to establish how the miR-2110/PTPN14/YAP1 pathway leads to endothelial cell injury in preeclampsia.

February 19, 2026Open Access

Circulating placental small extracellular vesicles miR-2110 depletion drives maternal-fetal endothelial injury in preeclampsia

Key Points

The research aims to establish how the miR-2110/PTPN14/YAP1 pathway leads to endothelial cell injury in preeclampsia.
Established the role of the miR-2110 regulatory pathway in endothelial injury
Investigated the sEVs-mediated communication in placental health
Examined the implications for cardiovascular risks in mothers and fetuses
Identified miR-2110 as a crucial mediator in endothelial injury
Linked placental ischemia to long-term cardiovascular risks for both mother and fetus
Proposed miR-2110 as an early diagnostic biomarker for preeclampsia

Abstract

We first established the role of the miR-2110/PTPN14/YAP1 pathway regulatory network in PE endothelial cell injury. This mechanism links placental ischemia with endothelial cell injury and long-term cardiovascular risks in both mother and fetus. Our study provides a comprehensive understanding of the sEVs-mediated placenta-endothelium communication axis in PE, and miR-2110 serves as both a mechanistic mediator and an early diagnostic biomarker, offering new insights for targeted interventions and improving adverse outcomes.

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Cite This Study

Wang et al. (Mon,) studied this question.

synapsesocial.com/papers/6996a7d3ecb39a600b3edea5 https://doi.org/https://doi.org/10.1186/s12964-026-02742-1

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