Véronique Witko‐Sarsat scite author profile

Evidence suggests an imbalance between antioxidant and oxidant-generating systems resulting in oxidative stress in uremic patients. As plasma proteins are critical targets for oxidants, we developed a novel spectrophotometric assay which allows to detect advanced oxidation protein products (AOPP) in uremic plasma. By size-exclusion chromatography AOPP are retrieved in two distinct peaks at 600 and below 80 kDa in uremic plasma, while no such peaks are found in control plasma. Further biochemical characterization revealed that AOPP are carried by oxidized plasma proteins, especially albumin and do not have oxidant properties. AOPP increased in a dose-dependent manner following in vitro exposure of plasma or purified human serum albumin (HSA) to hypochlorous acid. Advanced glycation end products of human serum albumin (AGE-HSA) also increased AOPP levels. In vivo, plasma level of AOPP was the highest in patients on hemodialysis, followed by those on peritoneal dialysis and by undialyzed patients with advanced chronic renal failure. AOPP levels correlated with plasma concentrations of dityrosine and AGE-pentosidine, as indices of oxidant-mediated protein damage, but not with thiobarbituric reactive substances as lipid peroxidation markers. A close correlation was also found between AOPP and neopterin levels, suggesting that AOPP could be part in the monocyte-mediated inflammatory disorders associated with uremia. In conclusion, we propose the measurement of AOPP as a reliable marker to estimate the degree of oxidant-mediated protein damage in uremic patients and to predict the potential efficacy of therapeutic strategies aimed at reducing such an oxidative stress.

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Neutrophils: Molecules, Functions and Pathophysiological Aspects

Witko‐Sarsat

Rieu

Descamps‐Latscha

et al. 2000

Laboratory Investigation

932

711

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Glutathione antioxidant system as a marker of oxidative stress in chronic renal failure

Ceballos-Picot

Witko‐Sarsat

Merad-Boudia

et al. 1996

Free Radical Biology and Medicine

339

234

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Iron Therapy, Advanced Oxidation Protein Products, and Carotid Artery Intima-Media Thickness in End-Stage Renal Disease

et al. 2002

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Background-Increased common carotid artery intima-media thickness (CCA-IMT) is a marker of early atherosclerosis.Low-grade inflammation is associated with the pathogenesis of atherosclerosis. Low-grade inflammation and increased CCA-IMT are observed in end-stage renal disease (ESRD). Oxidative stress is involved in uremia-related inflammation. Advanced oxidation protein products (AOPP) are markers of oxidant-mediated protein damage in ESRD. Intravenous iron given to patients on hemodialysis (HD) might induce oxidative stress. We investigated the relationships between AOPP, iron therapy, and CCA-IMT in stable HD patients. Methods and Results-Plasma AOPP and blood chemistry, including iron status, were analyzed in a cohort of 79 ESRD patients on HD. Measurements of CCA-IMT and CCA diameter, as assessed by B-mode ultrasonography, were obtained in 60 patients. AOPP levels were elevated in ESRD patients, and in univariate (rϭ0.42, PϽ0.0001) and multivariate analyses (rϭ0.38, PϽ0.001), they correlated with serum ferritin and with the intravenous iron dose received during the 12 months preceding the study (ferritin, PϽ0001; AOPP, PϽ0.01). Univariate and multivariate analyses identified the AOPP concentration as being significantly associated with CCA-IMT (Pϭ0.0197) and CCA wall-to-lumen ratio (rϭ0.560, PϽ0.0001). Independently of AOPP concentration, cumulative iron dose was positively related to CCA-IMT (Pϭ0.015) in patients Ͻ60 years. Conclusion-In ESRD patients, CCA-IMT and CCA wall-to-lumen ratio were associated with plasma AOPP, serum ferritin, and the annual intravenous iron dose administered. These findings support the concept of a role of oxidative stress in the early atherosclerosis of ESRD patients, which may be increased by the usually recommended doses of intravenous iron.

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Proliferating cell nuclear antigen acts as a cytoplasmic platform controlling human neutrophil survival

et al. 2010

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Oxidative stress and haemodialysis: role of inflammation and duration of dialysis treatment

Nguyen–Khoa¹,

Massy²,

Bandt³

et al. 2001

211

142

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

Witko‐Sarsat

Gausson

Nguyen

et al. 2003

Kidney International

211

134

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Bimodal distribution of proteinase 3 (PR3) surface expression reflects a constitutive heterogeneity in the polymorphonuclear neutrophil pool

Halbwachs‐Mecarelli¹,

Bessou²,

Lesavre³

et al. 1995

FEBS Letters

145

125

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