Hydroxytyrosol (HT) is a bioactive phenolic compound naturally present in olives and
extra virgin olive oil (EVOO) which is described as an antioxidant, antitumoral and antiangiogenic
molecule. Previous studies of semi-synthetic HT-derivatives presented the hydroxytyrosyl alkyl ether
HT-C6 as one of the most potent derivatives studied in the context of antioxidant, anti-platelet and
antiangiogenic assays, but its direct effect on inflammation was not reported. In this work, we use
RT-qPCR measure of gene expression, protein analysis by Western-blot and immunofluorescence
techniques, adhesion and migration functional assays and single-cell monitoring of reactive oxygen
species (ROS) in order to explore in vitro the ability of HT-C6 to interfere in the inflammatory response
of endothelial cells (ECs). Our results showed that HT-C6 strongly reduces the TNF- -induced
expression of vascular cell adhesion molecule 1 (VCAM1), intercellular cell adhesion molecule 1
(ICAM1), E-selectin (SELE), C-C motif chemokine ligand 2 and 5 (CCL2 and CCL5) in HUVECs,
impairing the chemotactic and adhesion potential of these cells towards THP-1 monocytes in vitro.
In this work, we define a mechanism of action underlying the anti-inflammatory effect of HT-C6,
which involves the abrogation of nuclear factor kappa B (NF- B) pathway activation in ECs. These
results, together with the ability of HT-C6 to reduce ROS formation in ECs, point to this compound
as a promising HT-derivative to be tested in the treatment of atherosclerosis.