| Literature DB >> 30135684 |
Nandor Gabor Than1,2,3,4,5,6, Roberto Romero1,2,7,8,9, Adi Laurentiu Tarca1,2,3,10, Katalin Adrienna Kekesi11, Yi Xu1,2, Zhonghui Xu1,2,12, Kata Juhasz4, Gaurav Bhatti1,2, Ron Joshua Leavitt13, Zsolt Gelencser4, Janos Palhalmi4, Tzu Hung Chung13, Balazs Andras Gyorffy11, Laszlo Orosz14, Amanda Demeter4, Anett Szecsi4, Eva Hunyadi-Gulyas15, Zsuzsanna Darula15, Attila Simor11, Katalin Eder16, Szilvia Szabo4,17, Vanessa Topping1,2, Haidy El-Azzamy1,2, Christopher LaJeunesse1,2, Andrea Balogh1,2,4, Gabor Szalai1,2,4, Susan Land9, Olga Torok14, Zhong Dong1,2, Ilona Kovalszky6, Andras Falus16, Hamutal Meiri18, Sorin Draghici9,19, Sonia S Hassan1,2,3,20, Tinnakorn Chaiworapongsa1,2,3, Manuel Krispin13, Martin Knöfler21, Offer Erez1,2,3,22, Graham J Burton23, Chong Jai Kim1,2,24,25, Gabor Juhasz11, Zoltan Papp5.
Abstract
Preeclampsia is a disease of the mother, fetus, and placenta, and the gaps in our understanding of the complex interactions among their respective disease pathways preclude successful treatment and prevention. The placenta has a key role in the pathogenesis of the terminal pathway characterized by exaggerated maternal systemic inflammation, generalized endothelial damage, hypertension, and proteinuria. This sine qua non of preeclampsia may be triggered by distinct underlying mechanisms that occur at early stages of pregnancy and induce different phenotypes. To gain insights into these molecular pathways, we employed a systems biology approach and integrated different "omics," clinical, placental, and functional data from patients with distinct phenotypes of preeclampsia. First trimester maternal blood proteomics uncovered an altered abundance of proteins of the renin-angiotensin and immune systems, complement, and coagulation cascades in patients with term or preterm preeclampsia. Moreover, first trimester maternal blood from preterm preeclamptic patients in vitro dysregulated trophoblastic gene expression. Placental transcriptomics of women with preterm preeclampsia identified distinct gene modules associated with maternal or fetal disease. Placental "virtual" liquid biopsy showed that the dysregulation of these disease gene modules originates during the first trimester. In vitro experiments on hub transcription factors of these gene modules demonstrated that DNA hypermethylation in the regulatory region of ZNF554 leads to gene down-regulation and impaired trophoblast invasion, while BCL6 and ARNT2 up-regulation sensitizes the trophoblast to ischemia, hallmarks of preterm preeclampsia. In summary, our data suggest that there are distinct maternal and placental disease pathways, and their interaction influences the clinical presentation of preeclampsia. The activation of maternal disease pathways can be detected in all phenotypes of preeclampsia earlier and upstream of placental dysfunction, not only downstream as described before, and distinct placental disease pathways are superimposed on these maternal pathways. This is a paradigm shift, which, in agreement with epidemiological studies, warrants for the central pathologic role of preexisting maternal diseases or perturbed maternal-fetal-placental immune interactions in preeclampsia. The description of these novel pathways in the "molecular phase" of preeclampsia and the identification of their hub molecules may enable timely molecular characterization of patients with distinct preeclampsia phenotypes.Entities:
Keywords: inflammation; ischemia; liquid biopsy; omics; placenta; pregnancy; systems biology; trophoblast invasion
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Year: 2018 PMID: 30135684 PMCID: PMC6092567 DOI: 10.3389/fimmu.2018.01661
Source DB: PubMed Journal: Front Immunol ISSN: 1664-3224 Impact factor: 7.561