Preeclampsia-Like Symptoms Induced in Mice by Fetoplacental Expression of STOX1 Are Reversed by Aspirin Treatment

Doridot, Ludivine; Passet, Bruno; Méhats, Céline; Rigourd, Virginie; Barbaux, Sandrine; Ducat, Aurélien; Mondon, Françoise; Vilotte, Marthe; Castille, Johan; Breuiller-Fouché, Michelle; Daniel, Nathalie; Provost, Fabienne Le; Bauchet, Anne-Laure; Baudrie, Véronique; Hertig, Alexandre; Buffat, Christophe; Simeoni, Umberto; Germain, Guy; Vilotte, Jean–Luc; Vaiman, Daniel

doi:10.1161/hypertensionaha.111.202994

Cited by 98 publications

(97 citation statements)

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“…In agreement with the implication of STOX1 in pre-eclampsia, overexpression of STOX1 was observed in early placental biopsies in gestations, eventually progressing to pre-eclampsia [GSE12767 in Founds et al (20)]. Furthermore, we induced pre-eclampsialike symptoms in two independent mouse strains overexpressing STOX1 (TgSTOX13 and TgSTOX42) (18). In the present study, we focused on the strain harboring the most severe phenotype, TgSTOX42.…”

Section: Discussionsupporting

confidence: 75%

“…RNA was extracted from placentas in TriZolÔ following classical protocols at 16.5 dpc from three different mice of each group as previously described (18). Quality control of the RNA, preparation of the probes, and hybridization on Nimblegen Mouse Expression Arrays MM8 were performed at the genom'IC platform (Cochin Institute, Paris, France) according to standard protocols.…”

Section: Mouse Placentas and Microarray Experimentsmentioning

confidence: 99%

“…Slides were incubated in blocking buffer (5% bovine serum albumin [BSA] in phosphate-buffered saline [PBS]) overnight at 4°C, then with the primary antibody for 1 h at room temperature (RT), and, finally, with the secondary antibody and 10 lg/ml of Hoechst 33342 for 1 h at RT. Atto488-conjugated anti-TOM22, anti-MAP1LC3B, and Immunohistochemistry of placentas was performed on WT or transgenic placentas (expressing the human STOX1 under the control of the cytomegalovirus promoter) (18). Mice were sacrificed near the end of gestation (E16.5).…”

Section: Reverse Transcription Quantitative Polymerase Chain Reactionmentioning

confidence: 99%

“…Overexpression of the storkhead box 1 (STOX1) transcription factor (71) induces transcriptome alteration, mimicking pre-eclampsia in choriocarcinoma JEG-3 cells, used as proxies for trophoblast cells (56), and induces a preeclampsia-like syndrome in vivo in a transgenic mouse model (18). Major transcriptome alterations in cells overexpressing STOX1 involve several cellular pathways, among which the mitochondrial function is highly represented (56).…”

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confidence: 99%

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Nitroso-Redox Balance and Mitochondrial Homeostasis Are Regulated bySTOX1, a Pre-Eclampsia-Associated Gene

Doridot

Châtre²,

Ducat³

et al. 2014

Antioxidants & Redox Signaling

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Aims: Storkhead box 1 (STOX1) is a winged-helix transcription factor that is implicated in the genetic forms of a high-prevalence human gestational disease, pre-eclampsia. STOX1 overexpression confers pre-eclampsia-like transcriptomic features to trophoblastic cell lines and pre-eclampsia symptoms to pregnant mice. The aim of this work was to evaluate the impact of STOX1 on free radical equilibrium and mitochondrial function, both in vitro and in vivo. Results: Transcriptome analysis of STOX1-transgenic versus nontransgenic placentas at 16.5 days of gestation revealed alterations of mitochondria-related pathways. Placentas overexpressing STOX1 displayed altered mitochondrial mass and were severely biased toward protein nitration, indicating nitrosoredox imbalance in vivo. Trophoblast cells overexpressing STOX1 displayed an increased mitochondrial activity at 20% O 2 and in hypoxia, despite reduction of the mitochondrial mass in the former. STOX1 overexpression is, therefore, associated with hyperactive mitochondria, resulting in increased free radical production. Moreover, nitric oxide (NO) production pathways were activated, resulting in peroxynitrite formation. At low oxygen pressure, STOX1 overexpression switched the free radical balance from reactive oxygen species (ROS) to reactive nitrogen species (RNS) in the placenta as well as in a trophoblast cell line. Innovation: In pre-eclamptic placentas, NO interacts with ROS and generates peroxynitrite and nitrated proteins as end products. This process will deprive the maternal organism of NO, a crucial vasodilator molecule. Conclusion: Our data posit STOX1 as a genetic switch in the ROS/RNS balance and suggest an explanation for elevated blood pressure in pre-eclampsia. Antioxid. Redox Signal. 21, 819-834.

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Section: Discussionsupporting

confidence: 75%

Section: Mouse Placentas and Microarray Experimentsmentioning

confidence: 99%

Section: Reverse Transcription Quantitative Polymerase Chain Reactionmentioning

confidence: 99%

mentioning

confidence: 99%

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Nitroso-Redox Balance and Mitochondrial Homeostasis Are Regulated bySTOX1, a Pre-Eclampsia-Associated Gene

Doridot

Châtre²,

Ducat³

et al. 2014

Antioxidants & Redox Signaling

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“…This approach can be used to monitor both normal and abnormal changes in CpG profiles as a function of gestational age, differentiation stage, genetic variation, and/or pregnancy complications with a placental origin or such disorders as preeclampsia, HELLP 3 (hemolysis, increased liver enzymes and low platelets) syndrome, and intrauterine growth restriction. For example, the STOX1 (storkhead box 1) gene, which is associated with the familial form of preeclampsia in the Netherlands (and experimentally confirmed in a transgenic mouse model), is mainly expressed by subtypes of trophoblast cells that contribute little, if anything, to the maternal plasma RNA pool (3,4 ). This low level of expression prevents or complicates STOX1 RNA profiling if one wants to assess the risk of women carrying the susceptibility allele.…”

Section: Presymptomatic Monitoring Of Fetal Well-beingmentioning

confidence: 99%

Maternal Plasma Bisulfite DNA Sequencing: Tomorrow Starts Today

Oudejans

2013

Clinical Chemistry

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Molecular Genetics of Preeclampsia

Williams

2016

Encyclopedia of Life Sciences

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Preeclampsia can occur during pregnancy affecting the health of both the mother and her baby during pregnancy. Preeclampsia is known to have a placental origin; however, the pathogenic changes which lead to the development of systemic endothelial dysfunction characteristic of the disorder remain to be determined. The key factors with an underlying genetic component, which are accepted as being important in the development of preeclampsia, include immune maladaptation, inadequate placentation, oxidative stress and thrombosis. For many years, it has been known that preeclampsia has a genetic component, and as such extensive genetic research has been carried out in this area using strategies including candidate gene studies and linkage analysis. Elucidating the exact genetic contribution to this disorder still remains a challenge owing to the complication of interactions between foetal and maternal genotypes, the environment and epistasis. Key Concepts The placenta is key to the development of preeclampsia. Inadequate trophoblast invasion is one of the primary stages involved in the pathogenesis of the severe early onset form of preeclampsia. Systemic endothelial dysfunction underlies the development of hypertension characteristic of preeclampsia. Understanding the genetic contribution to preeclampsia is complicated owing to the interaction between maternal and foetal genotypes. STOX1 and ACVR2A have been identified as potential positional candidate genes in preeclampsia.

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Preeclampsia-Like Symptoms Induced in Mice by Fetoplacental Expression of STOX1 Are Reversed by Aspirin Treatment

Cited by 98 publications

References 36 publications

Nitroso-Redox Balance and Mitochondrial Homeostasis Are Regulated bySTOX1, a Pre-Eclampsia-Associated Gene

Nitroso-Redox Balance and Mitochondrial Homeostasis Are Regulated bySTOX1, a Pre-Eclampsia-Associated Gene

Maternal Plasma Bisulfite DNA Sequencing: Tomorrow Starts Today

Molecular Genetics of Preeclampsia

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