Human and Mouse Eosinophils Differ in Their Ability to Biosynthesize Eicosanoids, Docosanoids, the Endocannabinoid 2-Arachidonoyl-glycerol and Its Congeners

Archambault, Anne-Sophie; Brassard, Julyanne; Bernatchez, Emilie; Martin, Cyril; Marzo, Vincenzo Di; Laviolette, Michel; Boulet, Louis‐Philippe; Blanchet, Marie‐Renée; Flamand, Nicolas

doi:10.3390/cells11010141

Cited by 4 publications

(1 citation statement)

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“…Due to the low cellular concentrations of 15-LO1, 15-LO2 and 12-LO in PMNL, no substantial amounts of AA-and DHA-derived SPMs were detected (Mainka et al, 2021). In contrast, human and mouse eosinophils which express ALOX15 biosynthesized docosanoids (14-HDHA, 17-HDHA) in the presence of DHA, but the resolvin levels were very low: RvD5 was the most prominent of these (Archambault et al, 2022). Noteworthy, the stimulation of eosinophils with platelet-activating factor (which increases intracellular Ca 2+ concentrations and thus 5lipoxygenase activity) did not increase docosanoids despite increasing leukotrienes.…”

Section: Lipoxin and Resolvin Formation In Human Pmnlmentioning

confidence: 97%

Formation, Signaling and Occurrence of Specialized Pro-Resolving Lipid Mediators—What is the Evidence so far?

et al. 2022

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Formation of specialized pro-resolving lipid mediators (SPMs) such as lipoxins or resolvins usually involves arachidonic acid 5-lipoxygenase (5-LO, ALOX5) and different types of arachidonic acid 12- and 15-lipoxygenating paralogues (15-LO1, ALOX15; 15-LO2, ALOX15B; 12-LO, ALOX12). Typically, SPMs are thought to be formed via consecutive steps of oxidation of polyenoic fatty acids such as arachidonic acid, eicosapentaenoic acid or docosahexaenoic acid. One hallmark of SPM formation is that reported levels of these lipid mediators are much lower than typical pro-inflammatory mediators including the monohydroxylated fatty acid derivatives (e.g., 5-HETE), leukotrienes or certain cyclooxygenase-derived prostaglandins. Thus, reliable detection and quantification of these metabolites is challenging. This paper is aimed at critically evaluating i) the proposed biosynthetic pathways of SPM formation, ii) the current knowledge on SPM receptors and their signaling cascades and iii) the analytical methods used to quantify these pro-resolving mediators in the context of their instability and their low concentrations. Based on current literature it can be concluded that i) there is at most, a low biosynthetic capacity for SPMs in human leukocytes. ii) The identity and the signaling of the proposed G-protein-coupled SPM receptors have not been supported by studies in knock-out mice and remain to be validated. iii) In humans, SPM levels were neither related to dietary supplementation with their ω-3 polyunsaturated fatty acid precursors nor were they formed during the resolution phase of an evoked inflammatory response. iv) The reported low SPM levels cannot be reliably quantified by means of the most commonly reported methodology. Overall, these questions regarding formation, signaling and occurrence of SPMs challenge their role as endogenous mediators of the resolution of inflammation.

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Section: Lipoxin and Resolvin Formation In Human Pmnlmentioning

confidence: 97%