Associations of Fully Automated CSF and Novel Plasma Biomarkers With Alzheimer Disease Neuropathology at Autopsy

Ashton Nicholas J; Blennow Kaj; Grothe Michel J; Zetterberg Henrik; Schöll Michael; Alzheimer’s Disease Neuroimaging Initiative; Moscoso Alexis; Lantero-Rodriguez Juan; Karikari Thomas K; Snellman Anniina

Associations of Fully Automated CSF and Novel Plasma Biomarkers With Alzheimer Disease Neuropathology at Autopsy

Ashton Nicholas J; Blennow Kaj; Grothe Michel J; Zetterberg Henrik; Schöll Michael; Alzheimer’s Disease Neuroimaging Initiative; Moscoso Alexis; Lantero-Rodriguez Juan; Karikari Thomas K; Snellman Anniina

Associations of Fully Automated CSF and Novel Plasma Biomarkers With Alzheimer Disease Neuropathology at Autopsy

Ashton Nicholas J

Blennow Kaj

Grothe Michel J

Zetterberg Henrik

Schöll Michael; Alzheimer’s Disease Neuroimaging Initiative

Moscoso Alexis

Lantero-Rodriguez Juan

Karikari Thomas K

Snellman Anniina

Katso/Avaa

Publisher's version (1.064Mb)

Lataukset:

Wolters Kluwer

doi:10.1212/WNL.0000000000012513

URI

https://n.neurology.org/content/early/2021/07/15/WNL.0000000000012513.long

Näytä kaikki kuvailutiedot

Julkaisun pysyvä osoite on:
https://urn.fi/URN:NBN:fi-fe2021093048778

Tiivistelmä

Objective: To study cerebrospinal fluid (CSF) biomarkers of Alzheimer's disease (AD) analyzed by fully automated Elecsys immunoassays in comparison to neuropathologic gold standards, and compare their accuracy to plasma phosphorylated tau (p-tau181) measured using a novel Simoa method.

Methods: We studied ante-mortem Elecsys-derived CSF biomarkers in 45 individuals who underwent standardized post-mortem assessments of AD and non-AD neuropathologic changes at autopsy. In a subset of 26 participants, we also analysed ante-mortem levels of plasma p-tau181 and neurofilament light (NfL). Reference biomarker values were obtained from 146 amyloid-PET-negative healthy controls (HC).

Results: All CSF biomarkers clearly distinguished pathology-confirmed AD dementia (N=27) from HC (AUCs=0.86-1.00). CSF total-tau (t-tau), p-tau181, and their ratios with Aβ_1-42, also accurately distinguished pathology-confirmed AD from non-AD dementia (N=8; AUCs=0.94-0.97). In pathology-specific analyses, intermediate-to-high Thal amyloid phases were best detected by CSF Aβ_1-42 (AUC[95% CI]=0.91[0.81-1]), while intermediate-to-high CERAD neuritic plaques and Braak tau stages were best detected by CSF p-tau181 (AUC=0.89[0.79-0.99] and 0.88[0.77-0.99], respectively). Optimal Elecsys biomarker cut-offs were derived at 1097/229/19 pg/ml for Aβ_1-42, t-tau, and p-tau181. In the plasma subsample, both plasma p-tau181 (AUC=0.91[0.86-0.96]) and NfL (AUC=0.93[0.87-0.99]) accurately distinguished pathology-confirmed AD (N=14) from HC. However, only p-tau181 distinguished AD from non-AD dementia cases (N=4; AUC=0.96[0.88-1.00]), and showed a similar, though weaker, pathologic specificity for neuritic plaques (AUC=0.75[0.52-0.98]) and Braak stage (AUC=0.71[0.44-0.98]) as CSF p-tau181.

Conclusions: Elecsys-derived CSF biomarkers detect AD neuropathologic changes with very high discriminative accuracy in-vivo. Preliminary findings support the use of plasma p-tau181 as an easily accessible and scalable biomarker of AD pathology.

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