Isolevuglandin-Type Lipid Aldehydes Induce the Inflammatory Response of Macrophages by Modifying Phosphatidylethanolamines and Activating the Receptor for Advanced Glycation Endproducts

Guo, Lilu; Chen, Zhongyi; Amarnath, Venkataraman; Yancey, Patricia G.; Lenten, Brian J. Van; Savage, Justin R.; Fazio, Sergio; Linton, MacRae F.; Davies, Sean S.

doi:10.1089/ars.2014.6078

Cited by 26 publications

(31 citation statements)

References 77 publications

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“…While 4-HNE typically induces JNK and p38 MAPK activation in HSCs [7,8] and in other cell types [39,52] it does not have significant effects on either Ras/ERK [7] or NF-kB [8]. Considering the lack of IsoLG-mediated NF-kB activation in hHSC while there is evidence that 15-E 2 -IsoLG strongly activates NF-kB in macrophages, this confirms previous observations suggesting a strong celltype dependency in the response to this mediator [30]. Similarly, we did not detect any significant activation of p38 MAPK, a known target of ER stress activation [20,47].…”

Section: Discussionsupporting

confidence: 87%

“…Overall, the most profound effect of hHSC exposure to IsoLG is an effect on the synthesis and secretion of pro-inflammatory cytokines/chemokines. Such direct pro-inflammatory and activating effects have also been demonstrated in immune cells such as macrophages [30], and dendritic cells [27]. Whilst HSC are not traditionally considered as the main hepatic immune cell type, they contribute to tissue inflammation by providing chemotactic signals that regulate their interaction with inflammatory cell types, as well as HSC themselves [53,54].…”

Section: Discussionmentioning

confidence: 99%

“…With respect to their potential role in liver disease, IsoLGs adducts have been described in livers of rodents exposed acutely to carbon tetrachloride [16], and chronically to ethanol [28,29], or high fat diet [30]. However, IsoLGs's effects on specific hepatic cell types and their potential contribution to disease pathogenesis have not been investigated.…”

Section: Longatomentioning

confidence: 99%

“…In other cell types, IsoLGs exposure promotes a proinflammatory phenotype, via upregulation of adhesion molecules, chemokines/cytokines, and transcription factors [20,27,30]. Therefore, we investigated if incubation of HSCs with IsoLGs had similar effects by measuring mRNA levels of multiple pro-inflammatory mediators [37].…”

Section: Determination Of the Range Of Bioactive Concentrations Of Ismentioning

confidence: 99%

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Reactive gamma-ketoaldehydes as novel activators of hepatic stellate cells in vitro

Longato

Andreola

Davies

et al. 2017

Free Radical Biology and Medicine

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Aims. Products of lipid oxidation, such as 4-hydroxynonenal (4-HNE), are key activators of hepatic stellate cells (HSC) to a pro-fibrogenic phenotype. Isolevuglandins (IsoLG) are a family of acyclic -ketoaldehydes formed through oxidation of arachidonic acid or as by-products of the cyclooxygenase pathway. IsoLGs are highly reactive aldehydes which are efficient at Longato 2 forming protein adducts and cross-links at concentrations 100-fold lower than 4-hydroxynonenal. Since the contribution of IsoLGs to liver injury has not been studied, we synthesized 15-E 2 -IsoLG and used it to investigate whether IsoLG could induce activation of HSC. Results. Primary human HSC were exposed to 15-E 2 -IsoLG for up to 48 hours.Exposure to 5 M 15-E 2 -IsoLG in HSCs promoted cytotoxicity and apoptosis. At non-cytotoxic doses (50 pM-500 nM) 15-E 2 -IsoLG promoted HSC activation, indicated by increased expression of α-SMA, sustained activation of ERK and JNK signaling pathways, and increased mRNA and/or protein expression of cytokines and chemokines, which was blocked by inhibitors of JNK and NF-kB. In addition, IsoLG promoted formation of reactive oxygen species, and induced an early activation of ER stress, followed by autophagy. Inhibition of autophagy partially reduced the pro-inflammatory effects of IsoLG, suggesting that it might serve as a cytoprotective response. Innovation. This study is the first to describe the biological effects of IsoLG in primary HSC, the main drivers of hepatic fibrosis. Conclusions. IsoLGs represent a newly identified class of activators of HSC in vitro, which are biologically active at concentrations as low as 500 pM, and are particularly effective at promoting a pro-inflammatory response and autophagy.

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Section: Discussionsupporting

confidence: 87%

Section: Discussionmentioning

confidence: 99%

Section: Longatomentioning

confidence: 99%

Section: Determination Of the Range Of Bioactive Concentrations Of Ismentioning

confidence: 99%

See 2 more Smart Citations

Reactive gamma-ketoaldehydes as novel activators of hepatic stellate cells in vitro

Longato

Andreola

Davies

et al. 2017

Free Radical Biology and Medicine

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“…Isolevuglandin-PE contributes to an NFkB-dependent inflammatory response in macrophages exposed to isolevuglandins by a mechanism involving binding to the receptor for advanced glycation end-products (RAGE). Moreover, isoLG adducts of PE were increased in hyperlipidemic and inflammatory conditions, such familial hypercholesterolemia in humans and high-fat diet induced obesity and hepatosteatosis in mice [75]. Analogous compounds called neuroketals can be formed from DHA via H 4 -neuroprostanes; these have been detected in brain tissue and age-related increases in protein adducts observed [76].…”

Section: Isolevuglandinsmentioning

confidence: 99%

Chemistry and analysis of HNE and other prominent carbonyl-containing lipid oxidation compounds

Sousa

Pitt

Spickett

2017

Free Radical Biology and Medicine

136

103

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The process of lipid oxidation generates a diverse array of small aldehydes and carbonyl-containing compounds, which may occur in free form or esterified within phospholipids and cholesterol esters. These aldehydes mostly result from fragmentation of fatty acyl chains following radical oxidation, and the products can be subdivided into alkanals, alkenals (usually D,β-unsaturated), γ-substituted alkenals and bis-aldehydes.Isolevuglandins are non-fragmented di-carbonyl compounds derived from H 2 -isoprostanes, and oxidation of the ω-3-fatty acid docosahexenoic acid yield analogous 22 carbon neuroketals. Non-radical oxidation by hypochlorous acid can generate D-chlorofatty aldehydes from plasmenyl phospholipids. Most of these compounds are reactive and have generally been considered as toxic products of a deleterious process. The reactivity is especially high for the D,β-unsaturated alkenals, such as acrolein and crotonaldehyde, and for γ-substituted alkenals, of which 4-hydroxy-2-nonenal and 4-oxo-2-nonenal are best Page | 2 known. Nevertheless, in recent years several previously neglected aldehydes have been investigated and also found to have significant reactivity and biological effects; notable examples are 4-hydroxy-2-hexenal and 4-hydroxy-dodecadienal. This has led to substantial interest in the biological effects of all of these lipid oxidation products and their roles in disease, including proposals that HNE is a second messenger or signalling molecule.However, it is becoming clear that many of the effects elicited by these compounds relate to their propensity for forming adducts with nucleophilic groups on proteins, DNA and specific phospholipids. This emphasizes the need for good analytical methods, not just for free lipid oxidation products but also for the resulting adducts with biomolecules. The most informative methods are those utilizing HPLC separations and mass spectrometry, although analysis of the wide variety of possible adducts is very challenging. Nevertheless, evidence for the occurrence of lipid-derived aldehyde adducts in biological and clinical samples is building, and offers an exciting area of future research. AbbreviationsAcr-dG, 1,N2-propanodeoxyguanosine; AGEs, advanced glycation end-product; ALEs, advanced lipoxidation end product; ApoB100, apolipoprotein B100; ApoE, apolipoprotein E; ARP, aldehyde reactive probe; AspN, endoproteinase AspN (flavastacin); βLG, β-lactoglobulin; BHZ, biotin hydrazide; BN-PAGE, blue native polyacrylamide gel

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Redox (phospho)lipidomics of signaling in inflammation and programmed cell death

Tyurina

Croix

Watkins

et al. 2019

Journal of Leukocyte Biology

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In addition to the known prominent role of polyunsaturated (phospho)lipids as structural blocks of biomembranes, there is an emerging understanding of another important function of these molecules as a highly diversified signaling language utilized for intra-and extracellular communications. Technological developments in high-resolution mass spectrometry facilitated the development of a new branch of metabolomics, redox lipidomics. Analysis of lipid peroxidation reactions has already identified specific enzymatic mechanisms responsible for the biosynthesis of several unique signals in response to inflammation and regulated cell death programs. Obtaining comprehensive information about millions of signals encoded by oxidized phospholipids, represented by thousands of interactive reactions and pleiotropic (patho)physiological effects, is a daunting task.However, there is still reasonable hope that significant discoveries, of at least some of the important contributors to the overall overwhelmingly complex network of interactions triggered by inflammation, will lead to the discovery of new small molecule regulators and therapeutic modalities. For example, suppression of the production of AA-derived pro-inflammatory mediators, HXA 3 and LTB 4, by an iPLA 2 inhibitor, R-BEL, mitigated injury associated with the activation of pro-inflammatory processes in animals exposed to whole-body irradiation. Further, technological developments promise to make redox lipidomics a powerful approach in the arsenal of diagnostic and therapeutic instruments for personalized medicine of inflammatory diseases and conditions. K E Y W O R D Seicosanoids, lipid mediators, lipoxygenase, Oxidized phospholipids, peroxidation, phospholipase A2, phospholipid hydrolysis

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Isolevuglandin-Type Lipid Aldehydes Induce the Inflammatory Response of Macrophages by Modifying Phosphatidylethanolamines and Activating the Receptor for Advanced Glycation Endproducts

Cited by 26 publications

References 77 publications

Reactive gamma-ketoaldehydes as novel activators of hepatic stellate cells in vitro

Reactive gamma-ketoaldehydes as novel activators of hepatic stellate cells in vitro

Chemistry and analysis of HNE and other prominent carbonyl-containing lipid oxidation compounds

Redox (phospho)lipidomics of signaling in inflammation and programmed cell death

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