Thus, an age-related decrease in NR2B expression could account for agerelated shortening of the excitatory postsynaptic potential duration of the NMDA channel.144,145 As mentioned above, overexpression of NR2B receptor subunits in transgenic mice enhances the activation of NMDA receptors, facilitating
Inhibitors,research,lifescience,medical synaptic potentiation as well as learning and memoir}’.22 This overexpression has also been reported to prevent, age-related decreases in GDC-0068 cost memory and learning performance. These results support, the hypothesis that age-related decreases in NMDA receptor function could account for age-related decreases in memory and learning. This suggests that strategies to prevent, those agerelated changes, or strategies to prevent, downstream or other events related Inhibitors,research,lifescience,medical to those changes, could have important therapeutic implications for the prevention or treatment of age-related memory impairments. NRHypo
hypothesis of AD In addition to age-related increases in NRHypo, it was recently shown in humans that a more severe degree of NRHypo is present in the AD brain than in agematched normal controls.97 Inhibitors,research,lifescience,medical Thus, in the aging human brain the stage may already be set for widespread corticolimbic neurodegeneration to occur. All that is required to explain why it occurs to a more severe degree in the AD brain than in the “normal” aging brain is to identify one or more adjunctive conditions peculiar to the AD brain that may serve as catalysts Inhibitors,research,lifescience,medical or promoters of the NRHypo state. In our animal model of NRHypo using otherwise healthy brain, no evidence of amyloidosis or amyloid plaque formation is observed. Therefore, we
propose that genetic or other predisposing factors peculiar to the AD condition are primarilyresponsible for the amyloidopathy in the AD brain and that when amyloidopathy occurs alongside NRHypo, the pathological process known as AD develops. How then does amyloidosis interact Inhibitors,research,lifescience,medical with NRHypo? Over the past decade, major strides have been made in discovering important genetic abnormalities in AD. Mutations on four different chromosomes, each of which can promote amyloidopathy, have now been identified as etiologic factors in familial AD Digestive enzyme and the role of apoE genotype as a risk factor in sporadic AD has been established. While recent research has elucidated the basic neurochemistry of beta-amyloid and it is clear that. abnormal deposition of beta-amyloid in the brain occurs early in AD, it. is not. at all clear how beta-amyloid deposition contributes to the neurodegenerative events in AD. Based on evidence that a severe degree of NRHypo is present in the human AD brain, that.