期刊
BRAIN
卷 144, 期 -, 页码 2826-2836出版社
OXFORD UNIV PRESS
DOI: 10.1093/brain/awab163
关键词
plasma biomarkers; amyloid-beta PET; tau PET; MRI; cognition
资金
- Swedish Research Council
- Knut and Alice Wallenberg foundation
- Marianne and Marcus Wallenberg foundation
- Strategic Research Area MultiPark (Multidisciplinary Research in Parkinson's disease) at Lund University
- Swedish Alzheimer Foundation
- Swedish Brain Foundation
- Strategic Research Area Neuroscience (StratNeuro)
- Center for Medical Innovation (CIMED)
- Parkinson foundation of Sweden
- Skane University Hospital Foundation
- Konung Gustaf V: S och Drottning Victorias Frimurarestiftelse
- Medical Faculty at Lund University, Region Skane
- Bundy Academy
- Swedish federal government under the ALF agreement
- GE Healthcare
- Swedish Research Council [2018-02201, 2017-00915, 2018-02532]
- Senior Researcher Faculty Position at Karolinska Institutet
- Strategic Research Programme in Neuroscience at Karolinska Institutet (Stratneuro Startup Grant)
- Center for Medical Innovation [20200695]
- Gamla Tjanarinnor and Stohnes
- Alzheimer Drug Discovery Foundation (ADDF), USA [RDAPB-201809-2016615]
- Swedish Alzheimer Foundation [AF-742881]
- Hjarnfonden, Sweden [FO2017-0243]
- Swedish government
- Swedish County Councils, the ALF-agreement [ALFGBG-715986]
- European Union [JPND2019-466-236]
- European Research Council [681712]
- Swedish State Support for Clinical Research [ALFGBG720931]
- UK Dementia Research Institute at UCL
- Vinnova [2018-02201] Funding Source: Vinnova
- Swedish Research Council [2018-02201] Funding Source: Swedish Research Council
Plasma biomarkers, particularly Aβ 42/40 and phosphorylated-tau217, can predict future Alzheimer's disease pathology in non-demented individuals, making them potential prognostic markers for clinical practice, research, and drug development.
It is currently unclear whether plasma biomarkers can be used as independent prognostic tools to predict changes associated with early Alzheimer's disease. In this study, we sought to address this question by assessing whether plasma biomarkers can predict changes in amyloid load, tau accumulation, brain atrophy and cognition in non-demented individuals. To achieve this, plasma amyloid-beta 42/40 (A beta 42/40), phosphorylated-tau181, phosphorylated-tau217 and neurofilament light were determined in 159 non-demented individuals, 123 patients with Alzheimer's disease dementia and 35 patients with a non-Alzheimer's dementia from the Swedish BioFINDER-2 study, who underwent longitudinal amyloid (F-18-flutemetamol) and tau (F-18-RO948) PET, structural MRI (T-1-weighted) and cognitive testing. Our univariate linear mixed effect models showed there were several significant associations between the plasma biomarkers with imaging and cognitive measures. However, when all biomarkers were included in the same multivariate linear mixed effect models, we found that increased longitudinal amyloid-PET signals were independently predicted by low baseline plasma A beta 42/40 (P = 0.012), whereas increased tau-PET signals, brain atrophy and worse cognition were independently predicted by high plasma phosphorylated-tau217 (P<0.004). These biomarkers performed equally well or better than the corresponding biomarkers measured in the CSF. In addition, they showed a similar performance to binary plasma biomarker values defined using the Youden index, which can be more easily implemented in the clinic. In addition, plasma A beta 42/40 and phosphorylated-tau217 did not predict longitudinal changes in patients with a non-Alzheimer's neurodegenerative disorder. In conclusion, our findings indicate that plasma A beta 42/40 and phosphorylated-tau217 could be useful in clinical practice, research and drug development as prognostic markers of future Alzheimer's disease pathology.
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