S-Thiolation Targets Albumin in Heart Failure

Brioschi, Marcos Leal; Gianazza, Erica; Mallia, Alice; Zoanni, Beatrice; Altomare, Alessandra; Fernández, Alma Martínez; Agostoni, Piergiuseppe; Aldini, Giancarlo; Banfi, Cristina

doi:10.3390/antiox9080763

Cited by 19 publications

(34 citation statements)

References 44 publications

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“…Still, when considering the incompatibility of the use of reducing agents with the analyses of mixed disulfides on Cys34, the addition of other analytical methods that complement bottom-up proteomics would be more desirable. Brioschi et al analyzed small thiol compounds originally bound to serum ALB as mixed disulfides [ 13 ]. These compounds were released by treating serum ALB with a reducing agent tris(2-carboxyethyl)phosphine, and they were then derivatized with 4-[2-(dimethylamino)ethylaminosulfonyl]-7-chloro-2,1,3-benzoxadiazole (DAABD-Cl).…”

Section: Analytical Chemistry Of Serum Alb Redox Statementioning

confidence: 99%

“…Binding affinities for lipid mediators also differs between reduced and oxidized serum ALB isoforms; proatherosclerotic lipids such as lysophosphatidylcholine and lysophosphatidic acid have higher affinities for oxidized ALB isoform, while anti-atherosclerotic mediators derived from eicosapentaenoic acid and docosahexaenoic acid possess higher affinities for reduced ALB isoform [ 12 ]. Furthermore, ALB oxidation (the increased HNA-1 level) was accompanied by decreased anti-oxidative activity as measured by a total radical-trapping antioxidant parameter assay [ 13 ]. The oxidation of biological components such as proteins, lipids, carbohydrates and DNA proceeds when anti-oxidative potential is attenuated.…”

Section: Introductionmentioning

confidence: 99%

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Serum Albumin Redox States: More Than Oxidative Stress Biomarker

et al. 2021

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Serum albumin is the most abundant circulating protein in mammals including humans. It has three isoforms according to the redox state of the free cysteine residue at position 34, named as mercaptalbumin (reduced albumin), non-mercaptalbumin-1 and -2 (oxidized albumin), respectively. The serum albumin redox state has long been viewed as a biomarker of systemic oxidative stress, as the redox state shifts to a more oxidized state in response to the severity of the pathological condition in various diseases such as liver diseases and renal failures. However, recent ex vivo studies revealed oxidized albumin per se could aggravate the pathological conditions. Furthermore, the possibility of the serum albumin redox state as a sensitive protein nutrition biomarker has also been demonstrated in a series of animal studies. A paradigm shift is thus ongoing in the research field of the serum albumin. This article provides an updated overview of analytical techniques for serum albumin redox state and its association with human health, focusing on recent findings.

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Section: Analytical Chemistry Of Serum Alb Redox Statementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Serum Albumin Redox States: More Than Oxidative Stress Biomarker

et al. 2021

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“…In healthy young persons, ≈70% and ≈30% of HSA presents Cys34 as a free sulfhydryl group and as a reversible mixed disulfide with other thiols of low molecular weight, respectively [ 109 ]. On the other hand, Brioschi et al found that S-thiolation of HSA was augmented in the plasma of heart failure patients, particularly in high severity cases (class III and class IV according to the New York Heart Association classification) [ 110 ]. In addition, the authors found that S-thiolated HSA correlated with deficient antioxidant activity in plasma, suggesting that S-thiolation promoted changes in HSA at the structure and function level [ 110 ].…”

Section: Other Modifications Of Albuminmentioning

confidence: 99%

“…On the other hand, Brioschi et al found that S-thiolation of HSA was augmented in the plasma of heart failure patients, particularly in high severity cases (class III and class IV according to the New York Heart Association classification) [ 110 ]. In addition, the authors found that S-thiolated HSA correlated with deficient antioxidant activity in plasma, suggesting that S-thiolation promoted changes in HSA at the structure and function level [ 110 ]. Similar results were found in eight end-stage renal disease patients with at least 3 months of hemodialysis, observing an increase in pre-dialysis S-thiolation levels of HSA compared to control patients.…”

Section: Other Modifications Of Albuminmentioning

confidence: 99%

Oxidized Albumin as a Mediator of Kidney Disease

et al. 2021

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Renal diseases are a global health concern, and nearly 24% of kidney disease patients are overweight or obese. Particularly, increased body mass index has been correlated with oxidative stress and urinary albumin excretion in kidney disease patients, also contributing to increased cardiovascular risk. Albumin is the main plasma protein and is able to partially cross the glomerular filtration barrier, being reabsorbed mainly by the proximal tubule through different mechanisms. However, it has been demonstrated that albumin suffers different posttranslational modifications, including oxidation, which appears to be tightly linked to kidney damage progression and is increased in obese patients. Plasma-oxidized albumin levels correlate with a decrease in estimated glomerular filtration rate and an increase in blood urea nitrogen in patients with chronic kidney disease. Moreover, oxidized albumin in kidney disease patients is independently correlated with higher plasma levels of transforming growth factor beta (TGF-β1), tumor necrosis factor (TNF-α), and interleukin (IL)-1β and IL-6. In addition, oxidized albumin exerts a direct effect on neutrophils by augmenting the levels of neutrophil gelatinase-associated lipocalin, a well-accepted biomarker for renal damage in patients and in different experimental settings. Moreover, it has been suggested that albumin oxidation occurs at early stages of chronic kidney disease, accelerating the patient requirements for dialytic treatment during disease progression. In this review, we summarize the evidence supporting the role of overweight- and obesity-induced oxidative stress as a critical factor for the progression of renal disease and cardiovascular morbimortality through albumin oxidation.

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“…quinones and unsaturated aldehydes) [ [31] , [32] , [33] , [34] , [35] ]. Increased levels of these modified forms are associated with smoking, aging, and multiple acute and chronic diseases [ [36] , [37] , [38] , [39] ].…”

Section: Introductionmentioning

confidence: 99%

Crosslinking of human plasma C-reactive protein to human serum albumin via disulfide bond oxidation

et al. 2021

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Inter- and intra-molecular crosslinks can generate protein dysfunction, and are associated with protein aggregate accumulation in aged and diseased tissues. Crosslinks formed between multiple amino acid side chains can be reversible or irreversible. Disulfides formed either enzymatically, or as a result of oxidant-mediated reactions, are a major class of reversible crosslinks. Whilst these are commonly generated via oxidation of Cys thiol groups, they are also formed by ‘oxidant-mediated thiol-disulfide reactions’ via initial disulfide oxidation to a thiosulfinate or zwitterionic peroxide, and subsequent reaction with another thiol including those on other proteins. This generates new intermolecular protein-protein crosslinks. Here we demonstrate that photooxidation, or reaction with the biological oxidants HOCl and ONOOH, of the single disulfide present in the major human plasma inflammatory protein, C-reactive protein (CRP) can give rise to reversible disulfide bond formation with human serum albumin (HSA). This occurs in an oxidant dose-, or illumination-time-, dependent manner. These CRP-HSA crosslinks are formed both in isolated protein systems, and in fresh human plasma samples containing high, but not low, levels of CRP. The inter-protein crosslinks which involve Cys36 of CRP and Cys34 of HSA, have been detected by both immunoblotting and mass spectrometry (MS). The yield of protein-protein crosslinks depends on the nature and extent of oxidant exposure, and can be reversed by dithiothreitol and tris(2-carboxyethyl)phosphine hydrochloride. These data indicate that oxidation of disulfide bonds in proteins can be a source of novel inter-protein crosslinks, which may help rationalize the accumulation of crosslinked proteins in aged and diseased tissues.

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S-Thiolation Targets Albumin in Heart Failure

Cited by 19 publications

References 44 publications

Serum Albumin Redox States: More Than Oxidative Stress Biomarker

Serum Albumin Redox States: More Than Oxidative Stress Biomarker

Oxidized Albumin as a Mediator of Kidney Disease

Crosslinking of human plasma C-reactive protein to human serum albumin via disulfide bond oxidation

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