AOPP-induced activation of human neutrophil and monocyte oxidative metabolism: A potential target for N-acetylcysteine treatment in dialysis patients

Witko‐Sarsat, Véronique; Gausson, Valérie; Nguyen, Anh‐Thu; Touam, Malik; Drüeke, Tilman B.; Santangelo, Francesco; Descamps‐Latscha, Béatrice

doi:10.1046/j.1523-1755.2003.00044.x

Cited by 214 publications

(151 citation statements)

References 41 publications

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“…The in vitro studies have demonstrated that AOPPs are capable of triggering the oxidative burst of human monocyte and neutrophil and stimulating leukocytes to produce more oxidants. [16,26,27] It seems reasonable to assume that oxidative stress in uremia can increase AOPP formation, and that AOPP accumulation may constitute a new molecular basis for enhanced oxidative stress. This positive feedback loop could amplify or maintain the oxidative stress in uremia.…”

Section: Discussionmentioning

confidence: 99%

Advanced Oxidation Protein Products Induce Vascular Calcification by Promoting Osteoblastic Trans-Differentiation of Smooth Muscle Cells via Oxidative Stress and ERK Pathway

et al. 2009

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Vascular calcification is an actively regulated process similar to bone formation. Advanced oxidation protein products (AOPPs) have been demonstrated to be novel markers of oxidantmediated protein damage. The present study investigated the role of AOPPs in inducing osteoblastic trans-differentiation and calcification of smooth muscle cells in vitro. We found that AOPPs directly increased the calcium deposition and expression of core binding factor-a1 (CBF-a1) and osteopontin (OPN) and significantly decreased SM-a-actin expression in human aortic smooth muscle cells (HASMCs). AOPPs increased intracellular oxidative stress, which was inhibited by vitamin E. Vitamin E also inhibited AOPP-induced calcium content and osteoblast differentiation of HASMCs. Furthermore, the inhibitor of ERK significantly suppressed the effects of AOPPs on calcification and osteoblast marker expression. These findings suggest that AOPPs induce vascular calcification by promoting osteoblast differentiation of smooth muscle cells via oxidative stress and ERK pathway.

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Section: Discussionmentioning

confidence: 99%

Advanced Oxidation Protein Products Induce Vascular Calcification by Promoting Osteoblastic Trans-Differentiation of Smooth Muscle Cells via Oxidative Stress and ERK Pathway

et al. 2009

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“…Before starting the therapy we determined AOPPs (ELISA Marc5+Max, Witko-Sarsat method 7,8 ), albumin cobalt binding (ACB) (COBAS MIRA+, Barr-Or method), glucose (ADVIA 1650, GOD-POD method), creatinine (ADVIA 1650, Jaffe method), urea (ADVIA 1650, enzyme method), ALT (ADVIA 1650, IFCC method), AST (ADVIA 1650, IFCC method), cholesterol (ADVIA 1650, enzyme method), LDL direct (ADVIA 1650, method with direct elimination), HDL (ADVIA 1650, method with direct elimination) and triglycerides (ADVIA 1650, enzyme) values in peripheral venous blood in all individuals.…”

Section: Methodsmentioning

confidence: 99%

The Antioxidant Acetylcysteine Reduces Oxidative Stress by Decreasing Level of Aopps

Lazarová¹,

Stejskal²,

Lacnák³

et al. 2004

BIOMED PAP

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Oxidative stress and especially its connection with many diseases has been discussed much recently. Among markers of oxidative stress there appear new and quite specific ones called advanced oxidation protein products (AOPPs). We tried to influence the level of AOPPs by an antioxidant therapy with N-acetylcysteine. Fourteen individuals with many cardiovascular risk factors were examined. All these patients were administered acetylcysteine (NAC)

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“…Despite the observation that proteins are highly susceptible to oxidative stress, there have been few reports of the production of oxidatively modified proteins in HD procedures. Measurement of markers of protein oxidation such as advanced oxidation protein products and carbonyl content have recently been performed to assess oxidative stress under pathological conditions (23)(24)(25)(26). In 2001, Himmelfarb et al (27) reported that the oxidation of albumin accounts for almost all of the excess plasma protein oxidation in uremic patients as demonstrated by SDS-PAGE and an immunoassay using a DNP antibody.…”

Section: Discussionmentioning

confidence: 99%

Effect of Olmesartan on Oxidative Stress in Hemodialysis Patients

et al. 2007

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AOPP-induced activation of human neutrophil and monocyte oxidative metabolism: A potential target for N-acetylcysteine treatment in dialysis patients

Abstract: This dual potential of NAC to inhibit phagocyte oxidative responses induced by HSA-AOPP without affecting those mediated by compounds mimicking pathogens supports the proposal of a therapeutic trial with NAC aimed at reducing oxidative stress-related inflammation in hemodialysis patients.

Cited by 214 publications

References 41 publications

Advanced Oxidation Protein Products Induce Vascular Calcification by Promoting Osteoblastic Trans-Differentiation of Smooth Muscle Cells via Oxidative Stress and ERK Pathway

Advanced Oxidation Protein Products Induce Vascular Calcification by Promoting Osteoblastic Trans-Differentiation of Smooth Muscle Cells via Oxidative Stress and ERK Pathway

The Antioxidant Acetylcysteine Reduces Oxidative Stress by Decreasing Level of Aopps

Effect of Olmesartan on Oxidative Stress in Hemodialysis Patients

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