Moscoso, A; Heeman, F; Raghavan, S; Costoya-Sánchez, A; Van Essen, M; Mainta, I; Camacho, V; ... Schöll, M; + view all Moscoso, A; Heeman, F; Raghavan, S; Costoya-Sánchez, A; Van Essen, M; Mainta, I; Camacho, V; Rodríguez-Fonseca, O; Silva-Rodríguez, J; Perissinotti, A; Gu, Y; Yun, J; Peretti, D; Ribaldi, F; Coomans, EM; Brum, WS; Grothe, MJ; Aguiar, P; Bischof, GN; Drzezga, A; Seo, SW; Villeneuve, S; Malpetti, M; O'Brien, JT; Rowe, JB; Van De Giessen, EM; Ossenkoppele, R; Jagust, WJ; Smith, R; Hansson, O; Frisoni, GB; Garibotto, V; Soleimani-Meigooni, DN; Carrillo, M; Dickerson, BC; La Joie, R; Rabinovici, GD; Apostolova, LG; Lamontagne, PJ; Pontecorvo, MJ; Johnson, KA; Sperling, RA; Weiner, MW; Petersen, RC; Jack, CR; Vemuri, P; Schöll, M; - view fewer (2025) Frequency and Clinical Outcomes Associated with Tau Positron Emission Tomography Positivity. Journal of the American Medical Association (JAMA) , 334 (3) pp. 229-242. 10.1001/jama.2025.7817.

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Abstract

Importance: Tau positron emission tomography (PET) allows in vivo detection of neurofibrillary tangles, a core neuropathologic feature of Alzheimer disease (AD). Objective: To provide estimates of the frequency of tau PET positivity and its associated risk of clinical outcomes. Design, Setting, and Participants: Longitudinal study using data pooled from 21 cohorts, comprising a convenience sample of 6514 participants from 13 countries, collected between January 2013 and June 2024. Cognitively unimpaired individuals and patients with a clinical diagnosis of mild cognitive impairment (MCI), AD dementia, or other neurodegenerative disorders were included. Exposures: Tau PET with flortaucipir F 18, amyloid-β (Aβ) PET, and clinical examinations. Tau PET scans were visually rated as positive according to a US Food and Drug Administration- and European Medicines Agency-approved method, designed to indicate the presence of advanced neurofibrillary tangle pathology (Braak stages V-VI). Main Outcomes and Measures: Frequency of tau PET positivity and absolute risk of clinical progression (eg, progression to MCI or dementia). Results: Among the 6514 participants (mean age, 69.5 years; 50.5% female), median follow-up time ranged from 1.5 to 4.0 years. Of 3487 cognitively unimpaired participants, 349 (9.8%) were tau PET positive; the estimated frequency of tau PET positivity was less than 1% in those aged younger than 50 years, and increased from 3% (95% CI, 2%-4%) at 60 years to 19% (95% CI, 16%-24%) at 90 years. Tau PET positivity frequency estimates increased across MCI and AD dementia clinical diagnoses (43% [95% CI, 41%-46%] and 79% [95% CI, 77%-82%] at 75 years, respectively). Most tau PET-positive individuals (92%) were also Aβ PET positive. Cognitively unimpaired participants who were positive for both Aβ PET and tau PET had a higher absolute risk of progression to MCI or dementia over the following 5 years (57% [95% CI, 45%-71%]) compared with both Aβ PET-positive/tau PET-negative (17% [95% CI, 13%-22%]) and Aβ PET-negative/tau PET-negative (6% [95% CI, 5%-8%]) individuals. Among participants with MCI at the time of the tau PET scan, an Aβ PET-positive/tau PET-positive profile was associated with a 5-year absolute risk of progression to dementia of 70% (95% CI, 59%-81%). Conclusions and Relevance: In a large convenience sample, a positive tau PET scan occurred at a nonnegligible rate among cognitively unimpaired individuals, and the combination of Aβ PET positivity and tau PET positivity was associated with a high risk of clinical progression in both preclinical and symptomatic stages of AD. These findings underscore the potential of tau PET as a biomarker for staging AD pathology.

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