Common Phenolic Metabolites of Flavonoids, but Not Their Unmetabolized Precursors, Reduce the Secretion of Vascular Cellular Adhesion Molecules by Human Endothelial Cells

Al-Shalmani; Amin; Andújar; Aydin; Barona; Blankenberg; Bondonno; Bornhoeft; Catalán; Chanet; Chen; Chen; Chen; Chen; Claude; Colin D Kay; Crozier; Curtis; Czank; Dall'Asta; David O'Hagan; de Ferrars; de Ferrars; di Gesso; Edwards; Emily F Warner; Faridi; Gandhi; Garton; Geleijnse; Geomela; Harasstani; Heeba; Juurlink; K Saki Raheem; Kakkar; Kay; Kay; Kjaergaard; Kling; Koga; Kwon; Ley; Livak; Lodi; Loke; Lotito; Lotito; Lusis; Luu; Maria A O'Connell; McKay; Min; Mink; Murota; Nabavi; Nakao; Olejarz; Pereira-Caro; Qingzhi Zhang; Ried; Rimbach; Rios; Rodriguez-Mateos; Rodriguez-Mateos; Schär; Serra; Sevgi; Sheng; Skoog; Urpi-Sarda; Videm; Vitaglione; Wang; Weseler; Winterbone; Xu; Zhang; Zhou; Zhu

research

Common Phenolic Metabolites of Flavonoids, but Not Their Unmetabolized Precursors, Reduce the Secretion of Vascular Cellular Adhesion Molecules by Human Endothelial Cells

Authors: Al-Shalmani
Amin
Andújar
Aydin
Barona
Blankenberg
Bondonno
Bornhoeft
Catalán
Chanet
Chen
Chen
Chen
Chen
Claude
Colin D Kay
Crozier
Curtis
Czank
Dall'Asta
David O'Hagan
de Ferrars
de Ferrars
di Gesso
Edwards
Emily F Warner
Faridi
Gandhi
Garton
Geleijnse
Geomela
Harasstani
Heeba
Juurlink
K Saki Raheem
Kakkar
Kay
Kay
Kjaergaard
Kling
Koga
Kwon
Ley
Livak
Lodi
Loke
Lotito
Lotito
Lusis
Luu
Maria A O'Connell
McKay
Min
Mink
Murota
Nabavi
Nakao
Olejarz
Pereira-Caro
Qingzhi Zhang
Ried
Rimbach
Rios
Rodriguez-Mateos
Rodriguez-Mateos
Schär
Serra
Sevgi
Sheng
Skoog
Urpi-Sarda
Videm
Vitaglione
Wang
Weseler
Winterbone
Xu
Zhang
Zhou
Zhu
Publication date: 1 January 2016
Publisher: 'American Society for Nutrition'
Doi

Abstract

Background: Flavonoids have been implicated in the prevention of cardiovascular disease; however, their mechanisms of action have yet to be elucidated, possibly because most previous in vitro studies have used supraphysiological concentrations of unmetabolized flavonoids, overlooking their more bioavailable phenolic metabolites. Objective: We aimed to explore the effects of phenolic metabolites and their precursor flavonoids at physiologically achievable concentrations, in isolation and combination, on soluble vascular cellular adhesion molecule-1 (sVCAM-1). Method: Fourteen phenolic acid metabolites and 6 flavonoids were screened at 1 μM for their relative effects on sVCAM-1 secretion by human umbilical vein endothelial cells stimulated with tumor necrosis factor alpha (TNF-α). The active metabolites were further studied for their response at different concentrations (0.01 μM–100 μM), structure-activity relationships, and effect on vascular cellular adhesion molecule (VCAM)-1 mRNA expression. In addition, the additive activity of the metabolites and flavonoids was investigated by screening 25 unique mixtures at cumulative equimolar concentrations of 1 μM. Results: Of the 20 compounds screened at 1 μM, inhibition of sVCAM-1 secretion was elicited by 4 phenolic metabolites, of which protocatechuic acid (PCA) was the most active (−17.2%, P = 0.05). Investigations into their responses at different concentrations showed that PCA significantly reduced sVCAM-1 15.2–36.5% between 1 and 100 μM, protocatechuic acid-3-sulfate and isovanillic acid reduced sVCAM-1 levels 12.2–54.7% between 10 and 100 μM, and protocatechuic acid-4-sulfate and isovanillic acid-3-glucuronide reduced sVCAM-1 secretion 27.6% and 42.8%, respectively, only at 100 μM. PCA demonstrated the strongest protein response and was therefore explored for its effect on VCAM-1 mRNA, where 78.4% inhibition was observed only after treatment with 100 μM PCA. Mixtures of the metabolites showed no activity toward sVCAM-1, suggesting no additive activity at 1 μM. Conclusions: The present findings suggest that metabolism of flavonoids increases their vascular efficacy, resulting in a diversity of structures of varying bioactivity in human endothelial cells