Classification of Preeclampsia According to Molecular Clusters with the Goal of Achieving Personalized Prevention

Overview

Journal J Reprod Immunol

Specialty Allergy & Immunology

Date 2023 Dec 23

PMID 38141514

Authors

Nandor Gabor Than

Roberto Romero

Mate Posta

Daniel Gyorffy

Gabor Szalai

Simona W Rossi

Andras Szilagyi

Petronella Hupuczi

Sandor Nagy

Olga Torok

Adi L Tarca

Offer Erez

Nandor Acs

Zoltan Papp

Affiliations

Soon will be listed here.

Abstract

The prevention of pre-eclampsia is difficult due to the syndromic nature and multiple underlying mechanisms of this severe complication of pregnancy. The current clinical distinction between early- and late-onset disease, although clinically useful, does not reflect the true nature and complexity of the pathologic processes leading to pre-eclampsia. The current gaps in knowledge on the heterogeneous molecular pathways of this syndrome and the lack of adequate, specific diagnostic methods are major obstacles to early screening and tailored preventive strategies. The development of novel diagnostic tools for detecting the activation of the identified disease pathways would enable early, accurate screening and personalized preventive therapies. We implemented a holistic approach that includes the utilization of different proteomic profiling methods of maternal plasma samples collected from various ethnic populations and the application of systems biology analysis to plasma proteomic, maternal demographic, clinical characteristic, and placental histopathologic data. This approach enabled the identification of four molecular subclasses of pre-eclampsia in which distinct and shared disease mechanisms are activated. The current review summarizes the results and conclusions from these studies and the research and clinical implications of our findings.

Citing Articles

Pulse Pressure as a Hemodynamic Parameter in Preeclampsia with Severe Features Accompanied by Fetal Growth Restriction.

Sampson R, Davis S, Wong R, Baranco N, Silverman R J Clin Med. 2024; 13(15).

PMID: 39124585 PMC: 11312723. DOI: 10.3390/jcm13154318.

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