Age-dependent changes in nitric oxide ((NO)-N-center dot) concentration dynamics may play a significant role in both decaying synaptic and metabolic functions in Alzheimer's disease (AD). This neuromodulator acts presynaptically to increase vesicle release and glutamatergic transmission and also regulates mitochondrial function. Under conditions of altered intracellular redox environment, (NO)-N-center dot may react and produce reactive species such as peroxynitrite. Using the triple transgenic mouse model of AD (3xTgAD), we investigated age-dependent changes in the glutamate-(NO)-N-center dot axis in the hippocampus. Direct measurement of (NO)-N-center dot concentration dynamics revealed a significant increase in N-methyl-D-aspartate type receptor-evoked peak (NO)-N-center dot in the 3xTgAD model at an early age. Aging produced a decrease in peak (NO)-N-center dot accompanied by significant decrease in production and decay rates in the transgenic model. Evaluation of energy metabolism revealed age-dependent decrease in basal oxygen consumption rate, a general decrease in mitochondrial oxidative phosphorylation parameters, and loss in mitochondrial sparing capacity in both genotypes. Finally, we observed age-dependent increase in 3-nitrotyrosine residues in the hippocampus, consistent with a putative shift in (NO)-N-center dot bioactivity toward oxidative chemistry associated with neurotoxicity.

• 出版日期2016-10