Neurons,especially axons,are metabolically demanding and energetically vulnerable during injury.However,the exact energy budget alterations that occur early after axon injury and the effects of these changes on neuronal survival remain unknown.Using a classic mouse model of optic nerve-crush injury,we found that traumatized optic nerves and retinas harbor the potential to mobilize two primary energetic machineries,glycolysis and oxidative phosphorylation,to satisfy the robustly increased adenosine triphosphate (ATP) demand.Further exploration of metabolic activation showed that mitochondrial oxidative phosphorylation was amplified over other pathways,which may lead to decreased retinal ganglion cell (RGC) survival despite its supplement to ATP production.Gene set enrichment analysis of a microarray (GSE32309) identified significant activation of oxidative phosphorylation in injured retinas from wild-type mice compared to those from mice with deletion of phosphatase and tensin homolog (PTEN),while PTEN-/-mice had more robust RGC survival.Therefore,we speculated that the oxidation-favoring metabolic pattern after optic nervecrush injury could be adverse for RGC survival.After redirecting metabolic flux toward glycolysis (magnifying the Warburg effect) using the drug meclizine,we successfully increased RGC survival.Thus,we provide novel insights into a potential bioenergetics-based strategy for neuroprotection.