Perinatal hypoxia-mediated neurodevelopment abnormalities in congenital heart disease mouse model

Renwei Chen; Haifan Wang; Liqin Zeng; Jiafei He; Xiaohan Liu; Xinting Ji; Paul Yao; Shuo Gu

doi:10.1186/s10020-025-01158-w

Molecular Medicine (Mar 2025)

Perinatal hypoxia-mediated neurodevelopment abnormalities in congenital heart disease mouse model

Renwei Chen,
Haifan Wang,
Liqin Zeng,
Jiafei He,
Xiaohan Liu,
Xinting Ji,
Paul Yao,
Shuo Gu

Affiliations

Renwei Chen: The First Affiliated Hospital, The First Clinical College, Key Laboratory of Emergency and Trauma of Ministry of Education, Hainan Medical University
Haifan Wang: Hainan Women and Children’s Medical Center, Hainan Medical University
Liqin Zeng: Department of Gynecology, Sun Yat-Sen University Affiliated No. 8 Hospital
Jiafei He: Hainan Women and Children’s Medical Center, Hainan Medical University
Xiaohan Liu: Department of Gynecology, Sun Yat-Sen University Affiliated No. 8 Hospital
Xinting Ji: The First Affiliated Hospital, The First Clinical College, Key Laboratory of Emergency and Trauma of Ministry of Education, Hainan Medical University
Paul Yao: Hainan Women and Children’s Medical Center, Hainan Medical University
Shuo Gu: The First Affiliated Hospital, The First Clinical College, Key Laboratory of Emergency and Trauma of Ministry of Education, Hainan Medical University

DOI: https://doi.org/10.1186/s10020-025-01158-w
Journal volume & issue: Vol. 31, no. 1
pp. 1 – 16

Abstract

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Abstract Background Cyanotic congenital heart disease (CHD) in children has been associated with neurodevelopmental abnormalities, although the underlying mechanisms remain largely unknown. Multiple factors are likely involved in this process. This research aims to explore the potential effects of hypoxia and vascular system-derived factors in neurodevelopmental outcomes in offspring. Methods Mouse aorta endothelial cells (MEC) and amygdala neurons were isolated to investigate the effects of hypoxia on pro-inflammatory cytokine release, gene expression, redox balance, mitochondrial function, and epigenetic modifications. A CHD mouse model was established to evaluate the impact of perinatal hypoxia on fetal brain development. Estrogen receptor β (ERβ) expression in endothelial cells was modulated using Tie2-driven lentivirus both in vitro and in vivo study to assess the vascular system’s contribution to hypoxia-mediated neurodevelopmental abnormalities. Results Hypoxia exposure, along with factors released from MEC, led to altered gene expression, oxidative stress, mitochondrial dysfunction, and epigenetic modifications in amygdala neurons. In the CHD mouse model, perinatal hypoxia resulted in compromised vascular function, altered gene expression, disrupted redox balance in brain tissues, and impaired behavioral outcomes in offspring. Prenatal expression of ERβ in endothelial cells partially ameliorated these neurodevelopmental abnormalities, while prenatal knockdown of ERβ mimicked the effects of perinatal hypoxia. Conclusions Hypoxia, combined with endothelial cell-derived factors, induces epigenetic changes in neurons. In the CHD mouse model, perinatal hypoxia causes vascular dysfunction, altered gene expression, and redox imbalance in brain tissues, leading to behavioral impairments in offspring. Prenatal expression of ERβ in endothelial cells mitigates these effects, suggesting that modulating gene expression in the vascular system during pregnancy could play a protective role against hypoxia-induced neurodevelopmental abnormalities in CHD.

Published in Molecular Medicine

ISSN: 1076-1551 (Print); 1528-3658 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology; Science: Chemistry: Organic chemistry: Biochemistry
Website: https://molmed.biomedcentral.com

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