Shared and unique effects of ApoEε4 and pathogenic gene mutation on cognition and imaging in preclinical familial Alzheimer’s disease

Abstract

AbstractBackgroundNeuropsychology and imaging changes have been reported in the preclinical stage of familial Alzheimer’s disease (FAD). This study investigated the effects of APOEε4 and known pathogenic gene mutation on different cognitive domains and circuit imaging markers in preclinical FAD.Method139 asymptomatic subjects in FAD families, including 26 APOEε4 carriers, 17 APP and 20 PS1 mutation carriers, and 76 control subjects, went through a series of neuropsychological tests and MRI scanning. Test scores and imaging measures including volumes, diffusion indices and functional connectivity (FC) of frontostriatal and hippocampus to posterior cingulate cortex pathways were compared between groups, and analyzed for correlation.ResultCompared with controls, APOEε4 group showed increased hippocampal volume and decreased FC of fronto‐caudate pathway (figure 1). APP group showed increased recall scores in auditory verbal learning test, decreased fiber number, increased radial diffusivity and FC of frontostriatal pathway (figure 1 & 2). All three genetic groups showed decreased fractional anisotropy of hippocampus to posterior cingulate cortex pathway (figure 1). These neuropsychological and imaging measures were able to discriminate genetic groups from controls, with areas under the curve from 0.733 to 0.837 (figure 3). Circuit imaging measures are differentially associated with scores in various cognitive scales in control and genetic groups.ConclusionThere are neuropsychological and imaging changes in the preclinical stage of FAD, some of which are shared by APOEε4 and known pathogenic gene mutation, while some are unique to different genetic groups. These findings are helpful for the early identification of Alzheimer’s disease, and for developing generalized and individualized prevention and intervention strategies.