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Therriault, Joseph; Pascoal, Tharick; Benedet, Andrea; Fernandez-Arias, Jaime; Wang, Tina; Berzgin, Gleb; Kang, Min Su; Lussier, Firoza; Chamoun, Mira; Savard, Melissa; Tissot, Cecile; Massarweh, Gassan; Soucy, Jean-Paul; Vitali, Paolo; Saha-Chaudhuri, Paramita; Gauthier, Serge; Rosa-Neto, Pedro — 2021-12-17 <p style="text-align:justify;"><b>Objective:</b> <span style="background:white;"> To assess the frequency of biologically-defined Alzheimer’s disease (AD) in relation to age, sex and <i>APOEε4</i>, as well as rates of discordance between clinically- and biologically defined AD. </span></p> <p style="text-align:justify;"><b>Methods:</b> <span style="background:white;">We assessed cognitively unimpaired (CU) elderly (n=166), amnestic MCI (n=77) and probable AD dementia (n=62) subjects who underwent evaluation by dementia specialists and neuropsychologists in addition to amyloi</span>d-PET with [¹⁸F]AZD4694<span style="background:white;"> and tau-PET with [¹⁸F]MK6240. Individuals were grouped according to their AD biomarker profile. Positive predictive value for biologically-defined AD was assessed in relation to clinical diagnosis. Frequency of AD biomarker profiles were assessed using logistic regressions with odds ratios and 95% CIs.</span></p> <p style="text-align:justify;"><b>Results:</b> <span style="background:white;">The clinical diagnosis of probable AD dementia demonstrated good agreement with biologically-defined AD (positive predictive value: 85.2%). 7.88% of CU elderly subjects were positive for both amyloid-PET and tau-PET. Frequency of biologically-defined AD increased with age (OR: 1.14; p&lt;0.0001) and frequency of <i>APOEε4</i> allele carriers (Single <i>ε4: </i>OR: 3.82; <i>p</i>&lt;0.0001; Double <i>ε4: </i>OR: 17.55, <i>p</i>&lt;0.0001). </span></p> <p style="text-align:justify;"><b>Discussion:</b> While we observed <span style="background:white;">strong, but not complete, agreement between clinically-defined “probable AD” dementia and biomarker positivity for both amyloid</span>-β<span style="background:white;"> and tau, we also observed that biologically-defined AD was not rare in CU elderly. A</span>bnormal tau-PET was almost exclusively observed in individuals with abnormal amyloid-PET. <span style="background:white;">Our results highlight that even in tertiary care memory clinics, detailed evaluation by dementia specialists systematically underestimates the frequency of biologically-defined AD and related entities. </span></p>