Cell-free DNA methylome analysis for early preeclampsia prediction

被引:0
|
作者
Marie De Borre
Huiwen Che
Qian Yu
Lore Lannoo
Kobe De Ridder
Leen Vancoillie
Pauline Dreesen
Mika Van Den Ackerveken
Mio Aerden
Eva Galle
Jeroen Breckpot
Joachim Van Keirsbilck
Wilfried Gyselaers
Koen Devriendt
Joris Robert Vermeesch
Kristel Van Calsteren
Bernard Thienpont
机构
[1] KU Leuven,Laboratory for Functional Epigenetics, Department of Human Genetics
[2] University Hospitals Leuven,Center for Human Genetics
[3] University of Leuven,Department of Obstetrics and Gynaecology
[4] University Hospitals Leuven,Faculty of Medicine and Life Science
[5] Hasselt University,Department of Obstetrics and Gynaecology
[6] St Jan’s Hospital,Department of Gynaecology
[7] Ziekenhuis Oost-Limburg,undefined
来源
Nature Medicine | 2023年 / 29卷
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摘要
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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页码:2206 / 2215
页数:9
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