Current State of Preeclampsia Mouse Models: Approaches, Relevance, and Standardization

Overview

Journal Front Physiol

Date 2021 Jul 19

PMID 34276401

Citations 13

Authors

Christopher A Waker

Melissa R Kaufman

Thomas L Brown

Affiliations

Soon will be listed here.

Abstract

Preeclampsia (PE) is a multisystemic, pregnancy-specific disorder and a leading cause of maternal and fetal death. PE is also associated with an increased risk for chronic morbidities later in life for mother and offspring. Abnormal placentation or placental function has been well-established as central to the genesis of PE; yet much remains to be determined about the factors involved in the development of this condition. Despite decades of investigation and many clinical trials, the only definitive treatment is parturition. To better understand the condition and identify potential targets preclinically, many approaches to simulate PE in mice have been developed and include mixed mouse strain crosses, genetic overexpression and knockout, exogenous agent administration, surgical manipulation, systemic adenoviral infection, and trophoblast-specific gene transfer. These models have been useful to investigate how biological perturbations identified in human PE are involved in the generation of PE-like symptoms and have improved the understanding of the molecular mechanisms underpinning the human condition. However, these approaches were characterized by a wide variety of physiological endpoints, which can make it difficult to compare effects across models and many of these approaches have aspects that lack physiological relevance to this human disorder and may interfere with therapeutic development. This report provides a comprehensive review of mouse models that exhibit PE-like symptoms and a proposed standardization of physiological characteristics for analysis in murine models of PE.

Citing Articles

Quantifying Molecular Changes in the Preeclamptic Rat Placenta with Targeted Contrast-Enhanced Ultrasound Imaging.

Shi L, Alencar A, Swan K, Lawrence D, Pridjian G, Bayer C Mol Imaging Biol. 2025; .

PMID: 40014198 DOI: 10.1007/s11307-025-01988-4.

Preeclampsia in mice carrying fetuses with APOL1 risk variants.

Yoshida T, Latt K, Shrivastav S, Lu H, Reidy K, Charlton J bioRxiv. 2025; .

PMID: 39803524 PMC: 11722342. DOI: 10.1101/2024.03.20.586039.

Placenta-tropic VEGF mRNA lipid nanoparticles ameliorate murine pre-eclampsia.

Swingle K, Hamilton A, Safford H, Geisler H, Thatte A, Palanki R Nature. 2024; 637(8045):412-421.

PMID: 39663452 DOI: 10.1038/s41586-024-08291-2.

Preeclampsia: Etiology, Pathophysiology, Risk Factors, Impact and Prevention: A Narrative Review.

Mustary M, Ansariadi , Syam A, Riskiyani S, Erika K, Moedjiono A Iran J Public Health. 2024; 53(11):2392-2403.

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Flow cytometric analysis of the murine placenta to evaluate nanoparticle platforms during pregnancy.

Swingle K, Hamilton A, Mitchell M Placenta. 2024; .

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