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Diagnosis of Alzheimer’s disease using plasma biomarkers adjusted to clinical probability

Authors
Therriault, J | Janelidze, S | Benedet, AL | Ashton, NJ | Arranz Martinez, J | Gonzalez-Escalante, A | Bellaver, B | Alcolea, D | Vrillon, A | Karim, H | Mielke, MM | Hong, CH  | Roh, HW  | Contador, J | Puig Pijoan, A | Algeciras-Schimnich, A | Vemuri, P | Graff-Radford, J | Lowe, VJ | Karikari, TK | Jonaitis, E | Brum, W | Tissot, C | Servaes, S | Rahmouni, N | Macedo, AC | Stevenson, J | Fernandez-Arias, J | Wang, YT | Woo, MS | Friese, MA | Jia, WL | Dumurgier, J | Hourregue, C | Cognat, E | Ferreira, PL | Vitali, P | Johnson, S | Pascoal, TA | Gauthier, S | Lleo, A | Paquet, C | Petersen, RC | Salmon, D | Mattsson-Carlgren, N | Palmqvist, S | Stomrud, E | Galasko, D | Son, SJ  | Zetterberg, H | Fortea, J | Suarez-Calvet, M | Jack, CR, Jr. | Blennow, K | Hansson, O | Rosa-Neto, P
Citation
Nature aging, 4(11). : 1529-1537, 2024
Journal Title
Nature aging
ISSN
2662-8465
Abstract
Recently approved anti-amyloid immunotherapies for Alzheimer’s disease (AD) require evidence of amyloid-β pathology from positron emission tomography (PET) or cerebrospinal fluid (CSF) before initiating treatment. Blood-based biomarkers promise to reduce the need for PET or CSF testing; however, their interpretation at the individual level and the circumstances requiring confirmatory testing are poorly understood. Individual-level interpretation of diagnostic test results requires knowledge of disease prevalence in relation to clinical presentation (clinical pretest probability). Here, in a study of 6,896 individuals evaluated from 11 cohort studies from six countries, we determined the positive and negative predictive value of five plasma biomarkers for amyloid-β pathology in cognitively impaired individuals in relation to clinical pretest probability. We observed that p-tau217 could rule in amyloid-β pathology in individuals with probable AD dementia (positive predictive value above 95%). In mild cognitive impairment, p-tau217 interpretation depended on patient age. Negative p-tau217 results could rule out amyloid-β pathology in individuals with non-AD dementia syndromes (negative predictive value between 90% and 99%). Our findings provide a framework for the individual-level interpretation of plasma biomarkers, suggesting that p-tau217 combined with clinical phenotyping can identify patients where amyloid-β pathology can be ruled in or out without the need for PET or CSF confirmatory testing.
MeSH

DOI
10.1038/s43587-024-00731-y
PMID
39533113
Appears in Collections:
Journal Papers > School of Medicine / Graduate School of Medicine > Psychiatry & Behavioural Sciences
Ajou Authors
노, 현웅  |  손, 상준  |  홍, 창형
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