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Metallomics [BCB/POMAM]

Jun 30 2023

Abstract

Copper (Cu) is essential for most organisms, but it can be poisonous in excess, through mechanisms such as protein aggregation, trans-metallation and oxidative stress. Latter could implicate the formation of potentially harmful Reactive Oxygen Species (ROS: O2•–, H2O2 and HO) via the redox cycling between Cu(II)/Cu(I) states in the presence of dioxygen and physiological reducing agents such as ascorbate (AscH), cysteine (Cys) and the tripeptide glutathione (GSH). Although the reactivity of Cu with these reductants has been previously investigated, the reactions taking place in a more physiologically-relevant mixture of these biomolecules are not known. Hence, we report here on the reactivity of Cu with binary and ternary mixtures of AscH, Cys and GSH. By measuring ascorbate and thiol oxidation, as well as HO formation, we show that Cu reacts preferentially with GSH and Cys, halting AscH oxidation and also HO release. This could be explained by the formation of Cu-thiolate clusters with both GSH and, as we first demonstrate here, Cys. Moreover, we observed a remarkable acceleration of Cu-catalysed GSH oxidation in the presence of Cys. We provide evidence that both thiol-disulfide exchange and the generated H2O2 contribute to this effect. Based on these findings, we speculate that Cu-induced oxidative stress may be mainly driven by GSH depletion and/or protein disulfide formation rather than by HO and envision a synergistic effect of Cys on Cu toxicity. 

 

 GA


Reference

Revisiting the pro-oxidant activity of copper: interplay of ascorbate, cysteine and glutathione

Falcone E, Stellato F, Vileno B, Bouraguba M, Lebrun V, Ilbert M, Morante S, Faller P.

Metallomics, 2023, DOI:  https://doi.org/10.1093/mtomcs/mfad040

 

Contact

Peter Faller (équipe BCB), Institut de Chimie de Strasbourg (UMR 7177).