Tert-butyl hydroperoxide (BHP), hydrogen peroxide and diamide caused a rapid and simultaneous release of glutathione disulfide (GSSG) and K⁺ in the isolated perfused rat liver. Both BHP-induced effluxes were suppressed by prior depletion of hepatic glutathione, but not by co-infusion of desferrioxamine which prevented lipid peroxidation and cell death. High K⁺ media decreased the GSSG efflux even though hepatic GSSG levels remained high. The GSSG and K⁺ effluxes were repeatable if cellular K⁺ recovered after a short BHP exposure. Ouabain inhibited the K⁺ re-uptake and decreased the response to repeated BHP challenge. Thus, sinusoidal efflux of GSSG under oxidative stress may be driven by a K⁺ gradient.