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      Effects of hemodialysis on plasma oxylipins

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          Abstract

          Chronic kidney disease (CKD) is an important risk factor for cardiovascular and all‐cause mortality. Survival rates among end‐stage renal disease (ESRD) hemodialysis patients are poor and most deaths are related to cardiovascular disease. Oxylipins constitute a family of oxygenated natural products, formed from fatty acid by pathways involving at least one step of dioxygen‐dependent oxidation. They are derived from polyunsaturated fatty acids (PUFAs) by cyclooxygenase (COX) enzymes, by lipoxygenases (LOX) enzymes, or by cytochrome P450 epoxygenase. Oxylipins have physiological significance and some could be of regulatory importance. The effects of decreased renal function and dialysis treatment on oxylipin metabolism are unknown. We studied 15 healthy persons and 15 CKD patients undergoing regular hemodialysis treatments and measured oxylipins (HPLC‐MS lipidomics) derived from cytochrome P450 (CYP) monooxygenase and lipoxygenase (LOX)/CYP ω/(ω‐1)‐hydroxylase pathways in circulating blood. We found that all four subclasses of CYP epoxy metabolites were increased after the dialysis treatment. Rather than resulting from altered soluble epoxide hydrolase (sEH) activity, the oxylipins were released and accumulated in the circulation. Furthermore, hemodialysis did not change the majority of LOX/CYP ω/(ω‐1)‐hydroxylase metabolites. Our data support the idea that oxylipin profiles discriminate ESRD patients from normal controls and are influenced by renal replacement therapies.

          Abstract

          To our knowledge, this is the first study to assess the impact of single hemodialysis treatment oxylipins in plasma using large‐scale lipidomics. We confirmed our hypothesis that the oxylipins status is influenced by hemodialysis treatment. Our data demonstrate that all four subclasses of CYP epoxy‐metabolites and a number of LOX/CYP ω/(ω‐1)‐hydroxylase metabolites are increased by the treatment. Moreover, ESRD patients undergoing regular dialysis show marked differences in plasma oxylipin profiles, that is, specific signatures, compared to normal control subjects.

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          Most cited references48

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          Identification of epoxyeicosatrienoic acids as endothelium-derived hyperpolarizing factors.

          Doris Campbell, D Gebremedhin, Jonathan D Harder (1996)
          Endothelial cells release several compounds, including prostacyclin, NO, and endothelium-derived hyperpolarizing factor (EDHF), that mediate the vascular effects of vasoactive hormones. The identity of EDHF remains unknown. Since arachidonic acid causes endothelium-dependent relaxations of coronary arteries through its metabolism to epoxyeicosatrienoic acids (EETs) by cytochrome P450, we wondered if the EETs represent EDHFs. Precontracted bovine coronary arteries relaxed in an endothelium-dependent manner to methacholine. The cytochrome P450 inhibitors, SKF 525A and miconazole, significantly attenuated these relaxations. They were also inhibited by tetraethylammonium (TEA),an inhibitor of Ca2+-activated K+ channels, and by high [K+]0 (20 mmol/L). Methacholine also caused hyperpolarization of coronary smooth muscle (-27 +/- 3.9 versus -40 +/- 5.1 mV), which was completely blocked by SKF 525A and miconazole. In vessels prelabeled with [3H] arachidonic acid, methacholine stimulated the release of 6-ketoprostaglandin F1alpha, 12-HETE, and the EETs. Arachidonic acid relaxed precontracted coronary arteries, which were also blocked by TEA, charybdotoxin, another Ca2+-activated K+ channel inhibitor, and high [K+]0. 14,15-EET, 11,12-EET, 8,9-EET, and 5,6-EET relaxed precontracted coronary vessels (EC50, 1 X 10(-6) mol/L). The four regioisomers were equally active. TEA, charybdotoxin, and high [K+]0 attenuated the EET relaxations. 11,12-EET hyperpolarized coronary smooth muscle cells from -37 +/- 0.2 to -59 +/- 0.3 mV. In the cell-attached mode of patch clamp, both 14,15-EET and 11,12-EET increased the open-state probability of a Ca2+-activated K+ channel in coronary smooth muscle cells. This effect was blocked by TEA and charybdotoxin. These data support the hypothesis that the EETs are EDHFs.
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            Epoxyeicosatrienoic acids (EETs): metabolism and biochemical function

            Arthur A Spector, Xiang Fang, Gary Snyder (2004)
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              Therapeutic potential of omega-3 fatty acid-derived epoxyeicosanoids in cardiovascular and inflammatory diseases.

              Karsten-Henrich Weylandt, Robert Fischer, Wolf-Hagen Schunck (2018)
              Numerous benefits have been attributed to dietary long-chain omega-3 polyunsaturated fatty acids (n-3 LC-PUFAs), including protection against cardiac arrhythmia, triglyceride-lowering, amelioration of inflammatory, and neurodegenerative disorders. This review covers recent findings indicating that a variety of these beneficial effects are mediated by "omega-3 epoxyeicosanoids", a class of novel n-3 LC-PUFA-derived lipid mediators, which are generated via the cytochrome P450 (CYP) epoxygenase pathway. CYP enzymes, previously identified as arachidonic acid (20:4n-6; AA) epoxygenases, accept eicosapentaenoic acid (20:5n-3; EPA) and docosahexaenoic acid (22:6n-3; DHA), the major fish oil n-3 LC-PUFAs, as efficient alternative substrates. In humans and rodents, dietary EPA/DHA supplementation causes a profound shift of the endogenous CYP-eicosanoid profile from AA- to EPA- and DHA-derived metabolites, increasing, in particular, the plasma and tissue levels of 17,18-epoxyeicosatetraenoic acid (17,18-EEQ) and 19,20-epoxydocosapentaenoic acid (19,20-EDP). Based on preclinical studies, these omega-3 epoxyeicosanoids display cardioprotective, vasodilatory, anti-inflammatory, and anti-allergic properties that contribute to the beneficial effects of n-3 LC-PUFAs in diverse disease conditions ranging from cardiac disease, bronchial disorders, and intraocular neovascularization, to allergic intestinal inflammation and inflammatory pain. Increasing evidence also suggests that background nutrition as well as genetic and disease state-related factors could limit the response to EPA/DHA-supplementation by reducing the formation and/or enhancing the degradation of omega-3 epoxyeicosanoids. Recently, metabolically robust synthetic analogs mimicking the biological activities of 17,18-EEQ have been developed. These drug candidates may overcome limitations of dietary EPA/DHA supplementation and provide novel options for the treatment of cardiovascular and inflammatory diseases.
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                Author and article information

                Contributors
                Benjamin Gollasch:
                ORCID: https://orcid.org/0000-0001-5267-518X
                benjamin.gollasch@charite.de
                Journal
                Journal ID (nlm-ta): Physiol Rep
                Journal ID (iso-abbrev): Physiol Rep
                Journal ID (doi): 10.1002/(ISSN)2051-817X
                Journal ID (publisher-id): PHY2
                Journal ID (hwp): physreports
                Title: Physiological Reports
                Publisher: John Wiley and Sons Inc. (Hoboken )
                ISSN (Electronic): 2051-817X
                Publication date (Electronic): 19 June 2020
                Publication date Collection: June 2020
                Volume: 8
                Issue: 12 ( doiID: 10.1002/phy2.v8.12 )
                Electronic Location Identifier: e14447
                Affiliations
                [ 1 ] Experimental and Clinical Research Center (ECRC), a joint institution between the Charité University Medicine and Max Delbrück Center (MDC) for Molecular Medicine Berlin‐Buch Germany
                [ 2 ] HELIOS Klinikum Berlin‐Buch Berlin Germany
                [ 3 ] Max Delbrück Center for Molecular Medicine (MDC) in the Helmholtz Association Berlin Germany
                [ 4 ] LIPIDOMIX GmbH Berlin Germany
                [ 5 ] Department of Geriatrics University of Greifswald University District Hospital Wolgast Greifswald Germany
                Author notes
                [*] [* ] Correspondence

                Benjamin Gollasch, Experimental and Clinical Research Center (ECRC), Lindenberger Weg 80, 13125 Berlin, Germany.

                Email: benjamin.gollasch@ 123456charite.de

                Author information
                https://orcid.org/0000-0001-5267-518X
                Article
                Publisher ID: PHY214447
                DOI: 10.14814/phy2.14447
                PMC ID: 7305238
                PubMed ID: 32562348
                SO-VID: 1f1bfbb4-675f-41fe-8548-96dfd2ea26e6
                Copyright © © 2020 The Authors. Physiological Reports published by Wiley Periodicals, Inc. on behalf of The Physiological Society and the American Physiological Society.
                License:

                This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

                History
                Date received : 28 January 2020
                Date revision received : 04 April 2020
                Date accepted : 24 April 2020
                Page count
                Figures: 1, Tables: 5, Pages: 24, Words: 10237
                Funding
                Funded by: Deutsche Forschungsgemeinschaft , open-funder-registry 10.13039/501100001659;
                Award ID: LU 435/13‐1
                Categories
                Subject: Renal Physiology
                Subject: Metabolic Pathways
                Subject: Circulation
                Subject: Original Research
                Subject: Original Research
                Custom metadata
                source-schema-version-number 2.0
                cover-date June 2020
                details-of-publishers-convertor Converter:WILEY_ML3GV2_TO_JATSPMC version:5.8.4 mode:remove_FC converted:19.06.2020

                Keywords: dialysis,eicosanoids,fatty acids,lipidomics,oxylipins
                Data availability:
                Keywords: dialysis, eicosanoids, fatty acids, lipidomics, oxylipins

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