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. 2023 Sep;29(9):2206-2215.
doi: 10.1038/s41591-023-02510-5. Epub 2023 Aug 28.

Cell-free DNA methylome analysis for early preeclampsia prediction

Marie De Borre  1   2 Huiwen Che #  1 Qian Yu #  1 Lore Lannoo  3 Kobe De Ridder  1 Leen Vancoillie  2 Pauline Dreesen  4 Mika Van Den Ackerveken  1 Mio Aerden  1   2 Eva Galle  1 Jeroen Breckpot  2 Joachim Van Keirsbilck  5 Wilfried Gyselaers  6 Koen Devriendt  2 Joris Robert Vermeesch  2 Kristel Van Calsteren  3 Bernard Thienpont  7
Affiliations

Cell-free DNA methylome analysis for early preeclampsia prediction

Marie De Borre et al. Nat Med. 2023 Sep.

Abstract

Preeclampsia (PE) is a leading cause for peripartal morbidity, especially if developing early in gestation. To enable prophylaxis in the prevention of PE, pregnancies at risk of PE must be identified early-in the first trimester. To identify at-risk pregnancies we profiled methylomes of plasma-derived, cell-free DNA from 498 pregnant women, of whom about one-third developed early-onset PE. We detected DNA methylation differences between control and PE pregnancies that enabled risk stratification at PE diagnosis but also presymptomatically, at around 12 weeks of gestation (range 9-14 weeks). The first-trimester risk prediction model was validated in an external cohort collected from two centers (area under the curve (AUC) = 0.75) and integrated with routinely available maternal risk factors (AUC = 0.85). The combined risk score correctly predicted 72% of patients with early-onset PE at 80% specificity. These preliminary results suggest that cell-free DNA methylation profiling is a promising tool for presymptomatic PE risk assessment, and has the potential to improve treatment and follow-up in the obstetric clinic.

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