Placental Tissue Calcification and Its Molecular Pathways in Female Patients with Late-Onset Preeclampsia

Biomolecules. 2024 Sep 30;14(10):1237. doi: 10.3390/biom14101237.

Abstract

Preeclampsia (PE) is a complex multisystem disease characterized by hypertension of sudden onset (>20 weeks' gestation) coupled with the presence of at least one additional complication, such as proteinuria, maternal organ dysfunction, or uteroplacental dysfunction. Hypertensive states during pregnancy carry life-threatening risks for both mother and baby. The pathogenesis of PE develops due to a dysfunctional placenta with aberrant architecture that releases factors contributing to endothelial dysfunction, an antiangiogenic state, increased oxidative stress, and maternal inflammatory responses. Previous studies have shown a correlation between grade 3 placental calcifications and an elevated risk of developing PE at term. However, little is known about the molecular pathways leading to placental calcification. In this work, we studied the gene and protein expression of c-Jun N-terminal kinase (JNK), Runt-related transcription factor 2 (RUNX2), osteocalcin (OSC), osteopontin (OSP), pigment epithelium-derived factor (PEDF), MSX-2/HOX8, SOX-9, WNT-1, and β-catenin in placental tissue from women with late-onset PE (LO-PE). In addition, we employed von Kossa staining to detect mineral deposits in placental tissues. Our results show a significant increase of all these components in placentas from women with LO-PE. Therefore, our study suggests that LO-PE may be associated with the activation of molecular pathways of placental calcification. These results could be the starting point for future research to describe the molecular mechanisms that promote placental calcification in PE and the development of therapeutic strategies directed against it.

Keywords: calcification; gene expression; late-onset preeclampsia (LO-PE); placenta; placental villi; tissue expression.

MeSH terms

  • Adult
  • Calcinosis* / genetics
  • Calcinosis* / metabolism
  • Calcinosis* / pathology
  • Female
  • Humans
  • Placenta* / metabolism
  • Placenta* / pathology
  • Pre-Eclampsia* / genetics
  • Pre-Eclampsia* / metabolism
  • Pre-Eclampsia* / pathology
  • Pregnancy

Grants and funding

This study (FIS-PI21/01244) was supported by the Instituto de Salud Carlos III (grant no. Estatal de I + D + I 2020–2027) and co-financed by the European Development Regional Fund “A way to achieve Europe”, as well as P2022/BMD-7321 (Comunidad de Madrid) and ProACapital, Halekulani S.L. and MJR.