Inflammation and oxidative stress are associated differently with endothelial function and arterial stiffness in healthy subjects and in patients with atherosclerosis

J Kals, P Kampus, M Kals, A Pulges… - … Journal of Clinical …, 2008 - Taylor & Francis
J Kals, P Kampus, M Kals, A Pulges, R Teesalu, K Zilmer, T Kullisaar, T Salum, J Eha
Scandinavian Journal of Clinical and Laboratory Investigation, 2008Taylor & Francis
Inflammation and oxidative stress (OxS) play key roles in atherogenesis; however, their
causal relationship is not yet completely understood. Much attention has been given to the
possibility that inflammation is a primary process of atherosclerosis and that OxS may be a
by‐product of the inflammatory process. We hypothesized, accordingly, that chronic systemic
inflammation affects endothelial vasomotor function in the subclinical condition, whereas
oxidative modifications are more involved in the structural stiffening of the arteries in …
Inflammation and oxidative stress (OxS) play key roles in atherogenesis; however, their causal relationship is not yet completely understood. Much attention has been given to the possibility that inflammation is a primary process of atherosclerosis and that OxS may be a by‐product of the inflammatory process. We hypothesized, accordingly, that chronic systemic inflammation affects endothelial vasomotor function in the subclinical condition, whereas oxidative modifications are more involved in the structural stiffening of the arteries in atherosclerosis. The aim of our study was to test this hypothesis. Endothelial function and arterial stiffness were assessed non‐invasively by pulse wave analysis, and blood/urinary samples were taken in 39 patients with peripheral arterial disease as well as in 34 controls. The patients showed significantly reduced endothelial function index (EFI) and increased augmentation index (AIx), as well as higher estimated aortic pulse wave velocity (PWV) and elevated values of the intercellular adhesion molecule‐1 (ICAM‐1), high sensitivity C‐reactive protein, myeloperoxidase and urinary 8‐iso‐prostaglandin F2a (F2‐IsoPs). There was an inverse association between EFI and ICAM‐1 (R = −0.44, p = 0.009) in the controls, but not in the patients. Augmentation index and estimated aortic PWV correlated with F2‐IsoPs only in the patients (R = 0.5, p = 0.001; R = −0.43, p = 0.006, respectively). After controlling for potential confounders, these associations remained significant. The study demonstrates that impairment of endothelial vasomotor capacity is affected by degree of inflammation in the subclinical condition, whereas arterial stiffening is determined by level of oxidative modifications in atherosclerosis.
Taylor & Francis Online