Pyruvate Protects Neurons against Hydrogen Peroxide-Induced Toxicity

Abstract

Hydrogen peroxide (H₂O₂) is suspected to be involved in numerous brain pathologies such as neurodegenerative diseases or in acute injury such as ischemia or trauma. In this study, we examined the ability of pyruvate to improve the survival of cultured striatal neurons exposed for 30 min to H₂O₂, as estimated 24 hr later by the 3-[4,5-dimethylthiazol-2-yl]−2,5-diphenyltetrazoliumbromide assay. Pyruvate strongly protected neurons against both H₂O₂added to the external medium and H₂O₂endogenously produced through the redox cycling of the experimental quinone menadione. The neuroprotective effect of pyruvate appeared to result rather from the ability of α-ketoacids to undergo nonenzymatic decarboxylation in the presence of H₂O₂than from an improvement of energy metabolism. Indeed, several other α-ketoacids, including α-ketobutyrate, which is not an energy substrate, reproduced the neuroprotective effect of pyruvate. In contrast, lactate, a neuronal energy substrate, did not protect neurons from H₂O₂. Optimal neuroprotection was achieved with relatively low concentrations of pyruvate (≤1 mm), whereas at high concentration (10 mm) pyruvate was ineffective. This paradox could result from the cytosolic acidification induced by the cotransport of pyruvate and protons into neurons. Indeed, cytosolic acidification both enhanced the H₂O₂-induced neurotoxicity and decreased the rate of pyruvate decarboxylation by H₂O₂. Together, these results indicate that pyruvate efficiently protects neurons against both exogenous and endogenous H₂O₂. Its low toxicity and its capacity to cross the blood–brain barrier open a new therapeutic perspective in brain pathologies in which H₂O₂is involved.