Alzheimer's disease pathology is attenuated in a CD38‐deficient mouse model

ObjectiveAlzheimer's disease (AD)‐associated dementia is due to tissue damage caused by amyloid β (Aβ) deposition within the brain and by accompanying neuroinflammation. The nicotinamide adenine dinucleotide (NAD) glycohydrolase CD38, which is expressed by neurons, astrocytes, and microglial cells, regulates inflammatory and repair processes in the brain and other tissues by degrading NAD and repressing the activity of other NAD‐consuming enzymes and by producing NAD‐derived metabolites that regulate calcium signaling and migration of inflammatory cells. Given the role of CD38 in neuroinflammation and repair, we examined the effect of CD38 deletion on AD pathology. MethodsWe crossed APPswePS1ΔE9 (APP.PS) mice with Cd38−/− mice to generate AD‐prone CD38‐deficient animals (APP.PS.Cd38−/−) and examined AD‐related phenotypes in both groups. ResultsAPP.PS.Cd38−/− mice exhibited significant reductions in Aβ plaque load and soluble Aβ levels compared to APP.PS mice, and this correlated with improved spatial learning. Although CD38 deficiency resulted in decreased microglia/macrophage (MM) accumulation, the transcription profile of the Cd38−/− and Cd38+/+ MM was similar, suggesting that the decreased Aβ burden in APP.PS.Cd38−/− mice was not due to alterations in MM activation/function. Instead, APP.PS.Cd38−/− neuronal cultures secreted less Aβ and this reduction was mimicked when APP.PS neuronal cultures were treated with inhibitors that blo...
Source: Annals of Neurology - Category: Neurology Authors: Tags: Research Article Source Type: research