Literature DB >> 27923813

The Chemical Basis of Thiol Addition to Nitro-conjugated Linoleic Acid, a Protective Cell-signaling Lipid.

Lucía Turell1,2, Darío A Vitturi3, E Laura Coitiño4, Lourdes Lebrato1,2, Matías N Möller2,5, Camila Sagasti4, Sonia R Salvatore3, Steven R Woodcock3, Beatriz Alvarez6,2, Francisco J Schopfer7.   

Abstract

Nitroalkene fatty acids are formed in vivo and exert protective and anti-inflammatory effects via reversible Michael addition to thiol-containing proteins in key signaling pathways. Nitro-conjugated linoleic acid (NO2-CLA) is preferentially formed, constitutes the most abundant nitrated fatty acid in humans, and contains two carbons that could potentially react with thiols, modulating signaling actions and levels. In this work, we examined the reactions of NO2-CLA with low molecular weight thiols (glutathione, cysteine, homocysteine, cysteinylglycine, and β-mercaptoethanol) and human serum albumin. Reactions followed reversible biphasic kinetics, consistent with the presence of two electrophilic centers in NO2-CLA located on the β- and δ-carbons with respect to the nitro group. The differential reactivity was confirmed by computational modeling of the electronic structure. The rates (kon and koff) and equilibrium constants for both reactions were determined for different thiols. LC-UV-Visible and LC-MS analyses showed that the fast reaction corresponds to β-adduct formation (the kinetic product), while the slow reaction corresponds to the formation of the δ-adduct (the thermodynamic product). The pH dependence of the rate constants, the correlation between intrinsic reactivity and thiol pKa, and the absence of deuterium solvent kinetic isotope effects suggested stepwise mechanisms with thiolate attack on NO2-CLA as rate-controlling step. Computational modeling supported the mechanism and revealed additional features of the transition states, anionic intermediates, and final neutral products. Importantly, the detection of cysteine-δ-adducts in human urine provided evidence for the biological relevance of this reaction. Finally, human serum albumin was found to bind NO2-CLA both non-covalently and to form covalent adducts at Cys-34, suggesting potential modes for systemic distribution. These results provide new insights into the chemical basis of NO2-CLA signaling actions.
© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  Michael addition; albumin; conjugated nitrolinoleic acid; elimination; fatty acid; kinetics; nitro fatty acid; nitroalkene fatty acid; sulfhydryl; thiol

Mesh:

Substances:

Year:  2016        PMID: 27923813      PMCID: PMC5270462          DOI: 10.1074/jbc.M116.756288

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


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3.  Electrophilic fatty acid nitroalkenes are systemically transported and distributed upon esterification to complex lipids.

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Review 6.  Nitro-fatty acid formation and metabolism.

Authors:  Gregory J Buchan; Gustavo Bonacci; Marco Fazzari; Sonia R Salvatore; Stacy Gelhaus Wendell
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7.  Transcriptomic sequencing reveals diverse adaptive gene expression responses of human vascular smooth muscle cells to nitro-conjugated linoleic acid.

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Review 9.  The discovery of nitro-fatty acids as products of metabolic and inflammatory reactions and mediators of adaptive cell signaling.

Authors:  Bruce A Freeman; Valerie B O'Donnell; Francisco J Schopfer
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10.  In situ generation, metabolism and immunomodulatory signaling actions of nitro-conjugated linoleic acid in a murine model of inflammation.

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Journal:  Redox Biol       Date:  2018-01-12       Impact factor: 11.799

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