Featured Article: Inhibition of glutathione synthesis distinctly alters mitochondrial and cytosolic redox poise

Author:

Kolossov Vladimir L1,Hanafin William P1,Beaudoin Jessica N12,Bica Denisa E1,DiLiberto Stephen J12,Kenis Paul JA13,Gaskins H Rex1245

Affiliation:

1. Institute for Genomic Biology, University of Illinois at Urbana-Champaign, Urbana, IL 61801, USA

2. Departments of Animal Sciences, University of Illinois at Urbana-Champaign, Urbana, IL 61801, USA

3. Chemical & Biomolecular Engineering, University of Illinois at Urbana-Champaign, Urbana, IL 61801, USA

4. Pathobiology, University of Illinois at Urbana-Champaign, Urbana, IL 61801, USA

5. Division of Nutritional Sciences, University of Illinois at Urbana-Champaign, Urbana, IL 61801, USA

Abstract

The glutathione couple GSH/GSSG is the most abundant cellular redox buffer and is not at equilibrium among intracellular compartments. Perturbation of glutathione poise has been associated with tumorigenesis; however, due to analytical limitations, the underlying mechanisms behind this relationship are poorly understood. In this regard, we have implemented a ratiometric, genetically encoded redox-sensitive green fluorescent protein fused to human glutaredoxin (Grx1-roGFP2) to monitor real-time glutathione redox potentials in the cytosol and mitochondrial matrix of tumorigenic and non-tumorigenic cells. First, we demonstrated that recovery time in both compartments depended upon the length of exposure to oxidative challenge with diamide, a thiol-oxidizing agent. We then monitored changes in glutathione poise in cytosolic and mitochondrial matrices following inhibition of glutathione (GSH) synthesis with L-buthionine sulphoximine (BSO). The mitochondrial matrix showed higher oxidation in the BSO-treated cells indicating distinct compartmental alterations in redox poise. Finally, the contributory role of the p53 protein in supporting cytosolic redox poise was demonstrated. Inactivation of the p53 pathway by expression of a dominant-negative p53 protein sensitized the cytosol to oxidation in BSO-treated tumor cells. As a result, both compartments of PF161-T+p53DD cells were equally oxidized ≈20 mV by inhibition of GSH synthesis. Conversely, mitochondrial oxidation was independent of p53 status in GSH-deficient tumor cells. Taken together, these findings indicate different redox requirements for the glutathione thiol/disulfide redox couple within the cytosol and mitochondria of resting cells and reveal distinct regulation of their redox poise in response to inhibition of glutathione biosynthesis.

Publisher

SAGE Publications

Subject

General Biochemistry, Genetics and Molecular Biology

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