2,3-Diarylxanthones as potential inhibitors of Arachidonic acid metabolic pathways

Santos, Clementina M.M.; Ribeiro, Daniela; Silva, Artur; Fernandes, Eduarda

http://hdl.handle.net/10198/14519

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Authors

Santos, Clementina M.M.

Ribeiro, Daniela

Silva, Artur

Fernandes, Eduarda

Abstract(s)

In response to an inflammatory stimulus, arachidonic acid (AA), the main polyunsaturated fatty acid present in the phospholipid layer of cell membranes, is released and metabolized to a series of eicosanoids. These bioactive lipid mediators of inflammation arise physiologically through the action of the enzymes 5-lipoxygenase (5-LOX) and cyclooxygenases (constitutive COX-1 and inducible COX-2). It is believed that dual inhibition of 5-LOX and COXs may have a higher beneficial impact in the treatment of inflammatory disorders rather than the inhibition of each enzyme. With this demand for new dual-acting anti-inflammatory agents, a range of 2,3-diarylxanthones were tested through their ability to interact in the AA metabolism. In vitro anti-inflammatory activity was evaluated through the inhibition of 5-LOX-catalyzed leukotriene B4 (LTB4) formation in human neutrophils and inhibition of COX-1- and COX-2-catalyzed prostaglandin E2 (PGE2) formation in human whole blood. The results showed that some of the studied arylxanthones were able to prevent LTB4 production in human neutrophils, in a concentration-dependent manner. The xanthone with a 2-catechol was the most active one (IC50 ∼ 9 μM). The more effective arylxanthones in preventing COX-1-catalyzed PGE2 production presented IC50 values from 1 to 7 μM, exhibiting a structural feature with at least one non-substituted aryl group. All the studied arylxanthones were ineffective to prevent the formation of PGE2 catalyzed by COX-2, up to the maximum concentration of 100 μM. The ability of the tested 2,3-diarylxanthones to interact with both 5-LOX and COX-1 pathways constitutes an important step in the research of novel dual-acting anti-inflammatory drugs.

Keywords

Xanthones 5-LOX COX-1 COX-2 Human neutrophils Human whole-blood assays

URI

http://hdl.handle.net/10198/14519

Citation

Santos, Clementina M.M.; Ribeiro, Daniela; Silva, Artur; Fernandes, Eduarda (2017). 2,3-Diarylxanthones as potential inhibitors of Arachidonic acid metabolic pathways. Inflammation. ISSN 0360-3997. 40:3, p. 956-964