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      High glutathionylation of placental endothelial nitric oxide synthase in preeclampsia

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          Abstract

          Decreased nitric oxide (NO) bioavailability plays a critical role in the pathophysiology of preeclampsia (PE). Recent evidence indicates that S-glutathionylation may occur on the endothelial nitric oxide synthase (eNOS), leading to eNOS uncoupling, characterized by a decreased NO production and an increased generation of superoxide anion (O 2 •–). We hypothesized that eNOS glutathionylation may occur in PE placentas and participate in eNOS dysfunction.

          The glutathionylation of eNOS was investigated in thirteen PE-affected patients and in nine normal pregnancies. Immunofluorescence, confocal microscopy and western-blot experiments carried out on eNOS immunoprecipitates, revealed a high level of eNOS glutathionylation in PE placentas, mostly reversed by dithiotreitol (DTT), thus indicative of S-glutathionylation. In order to investigate whether eNOS glutathionylation may alter trophoblast migration, an important event occurring during early placentation, cultured HTR-8/SVneo human trophoblasts (HTR8) were exposed either to low pO 2 (O 2 1%) or to pO 2 changes (O 2 1–20%), in order to generate oxidative stress. Trophoblasts exposed to low pO 2, did not undergo oxidative stress nor eNOS S-glutathionylation, and were able to generate NO and migrate in a wound closure model. In contrast, trophoblasts submitted to low/high pO 2 changes, exhibited oxidative stress and a (DTT reversible) S-glutathionylation of eNOS, associated with reduced NO production and migration. The autonomous production of NO seemed necessary for the migratory potential of HTR8, as suggested by the inhibitory effect of eNOS silencing by small interfering RNAs, and the eNOS inhibitor L-NAME, in low pO 2 conditions. Finally, the addition of the NO donor, NOC-18 (5 µM), restored in part the migration of HTR8, thereby emphasizing the role of NO in trophoblast homeostasis.

          In conclusion, the high level of eNOS S-glutathionylation in PE placentas provides new insights in the mechanism of eNOS dysfunction in this disease.

          Graphical abstract

          Highlights

          • eNOS is S-glutathionylated in preeclamptic placentas.

          • Oxidative stress evoked by pO 2 changes, triggers eNOS S-glutathionylation in HTR8.

          • pO 2 changes alter the invasive potential of HTR8 in the wound closure model.

          • The NO donor NOC-18 restores the invasive potential of HTR8.

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          Methods for detection of mitochondrial and cellular reactive oxygen species.

          Sergey Dikalov, David G. Harrison (2014)
          Mitochondrial and cellular reactive oxygen species (ROS) play important roles in both physiological and pathological processes. Different ROS, such as superoxide (O2(•-)), hydrogen peroxide, and peroxynitrite (ONOO(-)), stimulate distinct cell-signaling pathways and lead to diverse outcomes depending on their amount and subcellular localization. A variety of methods have been developed for ROS detection; however, many of these methods are not specific, do not allow subcellular localization, and can produce artifacts. In this review, we will critically analyze ROS detection and present advantages and the shortcomings of several available methods.
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            S-glutathionylation uncouples eNOS and regulates its cellular and vascular function.

            Chun-An Chen, Tse-Yao Wang, Saradhadevi Varadharaj (2010)
            Endothelial nitric oxide synthase (eNOS) is critical in the regulation of vascular function, and can generate both nitric oxide (NO) and superoxide (O(2)(•-)), which are key mediators of cellular signalling. In the presence of Ca(2+)/calmodulin, eNOS produces NO, endothelial-derived relaxing factor, from l-arginine (l-Arg) by means of electron transfer from NADPH through a flavin containing reductase domain to oxygen bound at the haem of an oxygenase domain, which also contains binding sites for tetrahydrobiopterin (BH(4)) and l-Arg. In the absence of BH(4), NO synthesis is abrogated and instead O(2)(•-) is generated. While NOS dysfunction occurs in diseases with redox stress, BH(4) repletion only partly restores NOS activity and NOS-dependent vasodilation. This suggests that there is an as yet unidentified redox-regulated mechanism controlling NOS function. Protein thiols can undergo S-glutathionylation, a reversible protein modification involved in cellular signalling and adaptation. Under oxidative stress, S-glutathionylation occurs through thiol-disulphide exchange with oxidized glutathione or reaction of oxidant-induced protein thiyl radicals with reduced glutathione. Cysteine residues are critical for the maintenance of eNOS function; we therefore speculated that oxidative stress could alter eNOS activity through S-glutathionylation. Here we show that S-glutathionylation of eNOS reversibly decreases NOS activity with an increase in O(2)(•-) generation primarily from the reductase, in which two highly conserved cysteine residues are identified as sites of S-glutathionylation and found to be critical for redox-regulation of eNOS function. We show that eNOS S-glutathionylation in endothelial cells, with loss of NO and gain of O(2)(•-) generation, is associated with impaired endothelium-dependent vasodilation. In hypertensive vessels, eNOS S-glutathionylation is increased with impaired endothelium-dependent vasodilation that is restored by thiol-specific reducing agents, which reverse this S-glutathionylation. Thus, S-glutathionylation of eNOS is a pivotal switch providing redox regulation of cellular signalling, endothelial function and vascular tone.
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              Endothelial dysfunction and preeclampsia: role of oxidative stress

              Lissette Sánchez-Aranguren, Carlos E. Prada, Carlos E. Riaño-Medina (2014)
              Preeclampsia (PE) is an often fatal pathology characterized by hypertension and proteinuria at the 20th week of gestation that affects 5–10% of the pregnancies. The problem is particularly important in developing countries in where the incidence of hypertensive disorders of pregnancy is higher and maternal mortality rates are 20 times higher than those reported in developed countries. Risk factors for the development of PE include obesity, insulin resistance and hyperlipidemia that stimulate inflammatory cytokine release and oxidative stress leading to endothelial dysfunction (ED). However, how all these clinical manifestations concur to develop PE is still not very well understood. The related poor trophoblast invasion and uteroplacental artery remodeling described in PE, increases reactive oxygen species (ROS), hypoxia and ED. Here we aim to review current literature from research showing the interplay between oxidative stress, ED and PE to the outcomes of current clinical trials aiming to prevent PE with antioxidant supplementation.
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                Author and article information

                Contributors
                Anne Negre-Salvayre
                Journal
                Journal ID (nlm-ta): Redox Biol
                Journal ID (iso-abbrev): Redox Biol
                Title: Redox Biology
                Publisher: Elsevier
                ISSN (Electronic): 2213-2317
                Publication date PMC-release: 26 January 2019
                Publication date Collection: April 2019
                Publication date (Electronic): 26 January 2019
                Volume: 22
                Electronic Location Identifier: 101126
                Affiliations
                [a ]Inserm U-1048, Université de Toulouse, France
                [b ]Pôle de gynécologie obstétrique, Hôpital Paule-de-Viguier, CHU de Toulouse, France
                [c ]Laboratory of Food Chemistry, Graduate School of Agricultural and Life Sciences, University of Tokyo, Japan
                Author notes
                [* ]Correspondence to: INSERM U-1048 – I2MC, CHU Rangueil, BP 84225, 31432 Toulouse Cedex 4, France. anne.negre-salvayre@ 123456inserm.fr
                [1]

                Equally contributors.

                Article
                Publisher ID: S2213-2317(19)30041-2 Publisher ID: 101126
                DOI: 10.1016/j.redox.2019.101126
                PMC ID: 6370867
                PubMed ID: 30738311
                SO-VID: d508a3d0-247e-40de-88dc-37c468365c72
                Copyright © © 2019 The Authors
                License:

                This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).

                History
                Date received : 9 January 2019
                Date accepted : 25 January 2019
                Categories
                Subject: Research Paper

                Keywords: no, nitric oxide,enos, endothelial nitric oxide synthase,inos, inducible nitric oxide synthase,o2•–, superoxide anion,ros, reactive oxygen species,gsh, reduced glutathione,gssg, oxidized glutathione,bh4, tetrahydrobiopterin,pe, preeclampsia,no,enos,s-glutathionylation,glutathione,oxidative stress,o2,pregnancy,trophoblast,migration,preeclampsia
                Data availability:
                Keywords: no, nitric oxide, enos, endothelial nitric oxide synthase, inos, inducible nitric oxide synthase, o2•–, superoxide anion, ros, reactive oxygen species, gsh, reduced glutathione, gssg, oxidized glutathione, bh4, tetrahydrobiopterin, pe, preeclampsia, no, enos, s-glutathionylation, glutathione, oxidative stress, o2, pregnancy, trophoblast, migration, preeclampsia

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