Accelerated cognitive decline and hippocampal volume loss in mild cognitive impaired carriers of Apolipoprotein‐E ε4

Background The ε4 allele of the Apolipoprotein‐E (APOE) gene is the major genetic risk factor for late‐onset Alzheimer’s disease (AD). APOE ε4 carriers represent around 45% of AD population, with each copy of APOE ε4 allele conferring increased risk for AD. Here, we aim to quantify disease progression during the early clinical stage of AD using imaging biomarkers to stratify patient populations for therapeutic interventions. Methods Data used in the preparation of this were obtained from the Alzheimer’s Disease Neuroimaging Initiative. CDR some of boxes (CDR‐SB), PET (amyloid load; Florbetapir), MRI (hippocampal volume) and APOE4 genotype were collected. Only MCI patients were included (MMSE=27.6±1.8 and global‐CDR=0.5±0.05). Available follow up data with at least 10 participants were included in the analysis. Results Data from 1021 participants with baseline MCI status were included in the study (110 ε4 homozygotes, 397 heterozygotes ε4). At baseline, CDR‐SB of non‐carriers and ε4 homozygotes was not different (p=0.24). The annual rate of cognitive decline in ε4 homozygotes (0.7 points per year; p=7e‐8) and heterozygotes ε4 (0.56 points per year; p=4e‐8) was 3.7 to 4.6 times greater than non‐carriers (0.15 points per year; p=0.00005). At baseline, hippocampal volume was significantly (p