Abstract
Flavonoids are compounds with a benzopyranic structure that exhibits multiple pharmacological activities. They are known for their venotonic activity, but their mechanism of action remains unclear. It is thought that, as this mechanism is mediated by prostaglandins, these compounds may interfere with the arachidonic acid (AA) cascade. These assays are designed to measure the antiplatelet aggregation capacity of quercetin, rutin, diosmetin, diosmin, and hidrosmin, as well as to evaluate a potential structure−activity ratio. In this paper, several studies on platelet aggregation at different concentrations (from 0.33 mM to 1.5 mM) of different flavone compounds are conducted, measuring platelet aggregation by impedance aggregometry, and the cyclooxygenase (COX) activity by metabolites generated, including the activity of the pure recombinant enzyme in the presence of these polyphenols. The results obtained showed that quercetin and diosmetin aglycones have a greater antiplatelet effect and inhibit the COX enzyme activity to a greater extent than their heterosides; however, the fact that greater inhibition of the pure recombinant enzyme was achieved by heterosides suggests that these compounds may have difficulty in crossing biological membranes. In any case, in view of the results obtained, it can be concluded that flavonoids could be useful as coadjuvants in the treatment of cardiovascular pathologies.
Highlights
Many papers on the properties of flavonoids have been written, yet they remain underrecognized [1]
Flavonoids were introduced in therapeutics for their vitamin P properties, due to their ability to improve capillary permeability when there was any alteration in permeability [3]
If prostaglandins controlled capillary permeability and flavonoids normalized it, it would be logical to suggest that these products would be interfering at a point in the arachidonic acid (AA) cascade, i.e., in the production of these prostaglandins (PG), so platelet aggregation is directly related to the production of AA metabolites [4,5]
Summary
Many papers on the properties of flavonoids have been written, yet they remain underrecognized [1]. Flavonoids were introduced in therapeutics for their vitamin P properties, due to their ability to improve capillary permeability when there was any alteration in permeability [3]. This effect appeared to be controlled by prostaglandins. The role of antiplatelet drugs is to prevent platelet activation either by inhibiting the platelet activation pathways or by stimulating inhibitory pathways [6]. These include cyclooxygenase (COX) blockers, as well as adenosine diphosphate (ADP) receptor antagonists and glycoprotein IIb/IIIa (GPIIb/IIIa) receptor antagonists [7]
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