Background: We aimed to validate the performance of an MRI-based machine learning derived Alzheimer's Disease-resemblance atrophy index (AD-RAI) in detecting preclinical and prodromal AD.Methods: A total of 62 subjects (mild cognitive impairment [MCI]=25, cognitively unimpaired [CU]=37) underwent MRI, 11 C-PIB, and 18 F-T807 PET. We investigated the performance of AD-RAI at the prespeci ed cutoff of ≥ 0.5 in detecting preclinical and prodromal AD and compared its performance with that of visual and volumetric hippocampal measures.Results: AD-RAI achieved the best metrics among all subjects (sensitivity 0.73, speci city 0.91, accuracy 87.10%) and among MCI subgroup (sensitivity 0.91, speci city 0.79, accuracy 84.00%) in detecting A+T+ subjects over other measures. Among CU subgroup, hippocampal volume (sensitivity 0.75, speci city 0.88, accuracy 86.49%) achieved a higher sensitivity than AD-RAI (sensitivity 0.25, speci city 0.97, accuracy 89.19%) in detecting preclinical AD.Conclusions: AD-RAI aids the detection of early AD, in particular at the prodromal stage.
BackgroundDetection of subjects at risk of developing dementia associated with Alzheimer's disease (AD) and intervention at the early stage provides the greatest opportunity in reducing the increasing dementia burden associated with AD, which is the commonest cause for dementia worldwide. The latest 2018 National Institute on Aging and Alzheimer's Association (NIA-AA) research framework de ned AD biologically by the presence of 2 core pathologic molecular biomarkers, beta-amyloid (A+) and neuro brillary tau (T+), rather than by the presence of cognitive impairment (1). With this de nition, subjects harboring A+T+ may exhibit a continuum of severity of cognitive impairment, ranging from cognitively unimpaired (CU) (i.e. preclinical AD), to mild cognitive impairment (MCI) (i.e. prodromal AD), to dementia (i.e. AD with dementia). The evolution from preclinical to prodromal AD, or from prodromal AD to AD with dementia may take several years and this slow transition provides an excellent window to implement strategies that may prevent conversion to dementia. This shift in paradigm (i.e. from reliance on clinical symptoms to molecular biomarkers, from focusing on dementia to pre-dementia stage) makes having an accurate in-vivo method in detecting AD biomarkers to be of great importance. At present, accurate in-vivo detection of beta-amyloid and neuro brillary tau is feasible with positron emission tomography (PET) and cerebrospinal uid (CSF) analysis. Studies comparing antemortem amyloid and tau PET and CSF analysis of beta-amyloid 1-42 and phosphorylated tau showed excellent correlation with post-mortem amyloid and tau burden (2-4). Both PET and/or CSF are currently considered as the gold standard in-vivo diagnostic tests for preclinical and prodromal AD.Apart from beta-amyloid and neuro brillary tau, the 2018 NIA-AA research framework also considers neurodegeneration (N) as another biomarker for AD (1). However, neurodegeneration is considered a
