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American Heart Association

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Final ID: Mo1009

Fatty Acid Binding Protein 4 as Potential Indicator for Gestational Diabetes Mellitus-Induced Fetal Endothelial Dysfunction

Abstract Body (Do not enter title and authors here): Introduction/Background: Gestational diabetes mellitus (GDM) is the most common complication during pregnancy. GDM is leading to an elevated risk for the development of cardiovascular diseases both in the mother and the child in later life. Previous studies have identified fatty acid-binding protein 4 (FABP4) as a prime candidate involved in the pathophysiology of GDM. Indeed, women with GDM exhibit elevated blood levels of FABP4, suggesting its potential role as a biomarker for endothelial dysfunction and cardiovascular risk assessment in GDM.
Research Question/Hypothesis: Does FABP4 affect the function of human endothelial cells from patients with GDM?
Goals/Aim: Our aim is a better understanding of the role of FABP4 in fetal endothelial dysfunction of patients with GDM and the development of potential therapeutic strategies.
Methods/Approach: Primary human umbilical vein endothelial cells (HUVECs) were isolated from umbilical cords obtained from normoglycemic and GDM pregnancies. Total mRNA from HUVECs was used for bulk RNA sequencing to compare gene expression pattern. HUVECs were subjected to functional analyses assessing proliferation, migration, NO and insulin signaling. Finally, human endothelial cells were exposed to high laminar flow (30 dyn/cm2) or simvastatin (10 nM) treatment to investigate their impact on FABP4 expression and endothelial function.
Results/Data: Bulk RNA sequencing data analysis revealed FABP4 as a gene overexpressed in GDM HUVECs compared to normoglycemic controls. Gene set enrichment analysis showed in addition an enrichment of genes involved in angiogenesis and Notch signaling pathways in human endothelial cells from GDM patients. GDM HUVECs had a significantly higher wound healing capacity compared to normoglycemic controls. The PI3K/AKT/mTOR pathway was enriched in GDM HUVECs. GDM HUVECs displayed impaired activation of AKT and eNOS (expression and phosphorylation) after stimulation with insulin, suggesting a possible insulin resistance. Finally, subjecting HUVECs to high laminar shear stress or simvastatin treatment caused a reduction of FABP4 mRNA expression and an increase of eNOS expression, indicating potential therapeutic strategies to improve endothelial function.
Conclusions: We provided evidence that FABP4 could be involved in fetal GDM-induced endothelial dysfunction. High laminar shear stress and medications activating eNOS signaling could protect the endothelium against the negative impact of FABP4 in GDM.
  • Villar Ballesteros, Maria De Leyre  ( UNIV OF TECHNOLOGY DRESDEN , Dresden , Germany )
  • Taylor, Paul  ( King's College London , London , United Kingdom )
  • Morawietz, Henning  ( UNIV OF TECHNOLOGY DRESDEN , Dresden , Germany )
  • Brendel, Heike  ( UNIV OF TECHNOLOGY DRESDEN , Dresden , Germany )
  • Hengst, Clara  ( UNIV OF TECHNOLOGY DRESDEN , Dresden , Germany )
  • Carstens, Philine Sophie  ( UNIV OF TECHNOLOGY DRESDEN , Dresden , Germany )
  • Effenberger, Deborah  ( UNIV OF TECHNOLOGY DRESDEN , Dresden , Germany )
  • Mittag, Jennifer  ( UNIV OF TECHNOLOGY DRESDEN , Dresden , Germany )
  • Giebe, Sindy  ( UNIV OF TECHNOLOGY DRESDEN , Dresden , Germany )
  • Fruehauf, Alexander  ( TU Dresden , Dresden , Germany )
  • Birdir, Cahit  ( TU Dresden , Dresden , Germany )
  • Author Disclosures:
    Maria de Leyre Villar Ballesteros: DO NOT have relevant financial relationships | Paul Taylor: No Answer | Henning Morawietz: DO NOT have relevant financial relationships | Heike Brendel: DO NOT have relevant financial relationships | Clara Hengst: DO NOT have relevant financial relationships | Philine Sophie Carstens: No Answer | Deborah Effenberger: No Answer | Jennifer Mittag: No Answer | Sindy Giebe: No Answer | Alexander Fruehauf: DO NOT have relevant financial relationships | Cahit Birdir: No Answer
Meeting Info:

Scientific Sessions 2024

2024

Chicago, Illinois

Session Info:

Cross-Talk in Cardiovascular and Metabolic Disorders

Monday, 11/18/2024 , 10:30AM - 11:30AM

Abstract Poster Session

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