Characterization of LY231617 Protection Against Hydrogen Peroxide Toxicity

Abstract

: The compound LY231617 {2,6‐bis(1,1‐dimethylethyl)‐4‐[[(1‐ethyl)amino]methyl]phenol hydrochloride} has been reported to afford significant neuroprotection against hydrogen peroxide (H₂O₂)‐induced toxicity in vitro and global ischemia in vivo. We now report on further mechanistic studies of H₂O₂ toxicity and protection by LY231617. Brief exposure to H₂O₂ (15 min) elicited an oxidative insult comparable with that generated by overnight treatment. H₂O₂‐mediated cellular degeneration was characterized using lactate dehydrogenase (LDH) release, changes in total glutathione, and a new marker of oxidative stress, 8‐epiprostaglandin F_2α (8‐isoprostane). LY231617 attenuated H₂O₂‐mediated degeneration under a variety of exposure conditions, including a more clinically relevant posttreatment paradigm. Levels of 8‐isoprostane paralleled LDH release under various treatment paradigms of 100 μM H₂O₂± 5 μM drug. In contrast, despite affording significant protection, LY231617 had modest to no effects on cellular levels of glutathione. Taken together, these results are consistent with a membrane site of action for LY231617 and suggest that the compound affords cytoprotection via its antioxidant properties.