What question did this study set out to answer?

To investigate the role of albumin as a dynamic regulator of polysulfides and redox status in various conditions.

June 4, 2026Open Access

Albumin as a dynamic extracellular redox regulator: from Cys34 oxidation biomarkers to polysulfide-mediated homeostatic mechanisms and clinical applications

Key Points

To investigate the role of albumin as a dynamic regulator of polysulfides and redox status in various conditions.
Quantification of albumin polysulfides using the Elimination Method for Sulfide from Polysulfide
Analysis of oxidative stress in chronic kidney disease and hepatitis
Evaluation of drug-binding capacity and scavenging activity of albumin under different conditions.
Albumin polysulfides are significantly depleted in chronic kidney disease and early hepatitis (exact metrics not provided)
Depletion of polysulfides impairs drug-binding capacity and reactive oxygen species scavenging activity
These findings suggest that modulating albumin polysulfides could enhance therapeutic efficacy.

Abstract

> 1) across multiple intramolecular cysteine bridges. Quantified using the newly developed Elimination Method for Sulfide from Polysulfide, albumin polysulfides are dynamically regulated by oxidative stress and are significantly depleted in chronic kidney disease and early hepatitis, even when conventional Cys34-based markers remain unchanged. Polysulfide depletion impairs both Site II drug-binding capacity and reactive oxygen species scavenging activity, with direct implications for pharmacokinetics and therapeutic efficacy. These findings collectively reframe HSA as a dynamic polysulfide reservoir and extracellular redox regulator, highlighting albumin polysulfide modulation as a compelling emerging therapeutic strategy.

Albumin as a dynamic extracellular redox regulator: from Cys34 oxidation biomarkers to polysulfide-mediated homeostatic mechanisms and clinical applications

Key Points

Abstract

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