Détail du document
Identifiant

oai:pubmedcentral.nih.gov:1011...

Sujet
Original Article
Auteur
Janelidze, Shorena Bali, Divya Ashton, Nicholas J Barthélemy, Nicolas R Vanbrabant, Jeroen Stoops, Erik Vanmechelen, Eugeen He, Yingxin Dolado, Anna Orduña Triana-Baltzer, Gallen Pontecorvo, Michael J Zetterberg, Henrik Kolb, Hartmuth Vandijck, Manu Blennow, Kaj Bateman, Randall J Hansson, Oskar
Langue
en
Editeur

Oxford University Press

Catégorie

Brain

Année

2022

Date de référencement

14/12/2023

Mots clés
biomarkers p-tau231 adx janss range baseline measured simoa ugot splex 0 diff using p-tau217 developed csf assays lilly alzheimer immunoassay auc washu dementia
Métrique

Résumé

Plasma phospho-tau (p-tau) species have emerged as the most promising blood-based biomarkers of Alzheimer's disease.

Here, we performed a head-to-head comparison of p-tau181, p-tau217 and p-tau231 measured using 10 assays to detect abnormal brain amyloid-β (Aβ) status and predict future progression to Alzheimer's dementia.

The study included 135 patients with baseline diagnosis of mild cognitive impairment (mean age 72.4 years; 60.7% women) who were followed for an average of 4.9 years.

Seventy-one participants had abnormal Aβ-status (i.e. abnormal CSF Aβ(42/40)) at baseline; and 45 of these Aβ-positive participants progressed to Alzheimer's dementia during follow-up.

P-tau concentrations were determined in baseline plasma and CSF.

P-tau217 and p-tau181 were both measured using immunoassays developed by Lilly Research Laboratories (Lilly) and mass spectrometry assays developed at Washington University (WashU).

P-tau217 was also analysed using Simoa immunoassay developed by Janssen Research and Development (Janss).

P-tau181 was measured using Simoa immunoassay from ADxNeurosciences (ADx), Lumipulse immunoassay from Fujirebio (Fuji) and Splex immunoassay from Mesoscale Discovery (Splex).

Both p-tau181 and p-tau231 were quantified using Simoa immunoassay developed at the University of Gothenburg (UGOT).

We found that the mass spectrometry-based p-tau217 (p-tau217(WashU)) exhibited significantly better performance than all other plasma p-tau biomarkers when detecting abnormal Aβ status [area under curve (AUC) = 0.947; P(diff) < 0.015] or progression to Alzheimer's dementia (AUC = 0.932; P(diff) < 0.027).

Among immunoassays, p-tau217(Lilly) had the highest AUCs (0.886–0.889), which was not significantly different from the AUCs of p-tau217(Janss), p-tau181(ADx) and p-tau181(WashU) (AUC(range) 0.835–0.872; P(diff) > 0.09), but higher compared with AUC of p-tau231(UGOT), p-tau181(Lilly), p-tau181(UGOT), p-tau181(Fuji) and p-tau181(Splex) (AUC(range) 0.642–0.813; P(diff) ≤ 0.029).

Correlations between plasma and CSF values were strongest for p-tau217(WashU) (R = 0.891) followed by p-tau217(Lilly) (R = 0.755; P(diff) = 0.003 versus p-tau217(WashU)) and weak to moderate for the rest of the p-tau biomarkers (R(range) 0.320–0.669).

In conclusion, our findings suggest that among all tested plasma p-tau assays, mass spectrometry-based measures of p-tau217 perform best when identifying mild cognitive impairment patients with abnormal brain Aβ or those who will subsequently progress to Alzheimer's dementia.

Several other assays (p-tau217(Lilly), p-tau217(Janss), p-tau181(ADx) and p-tau181(WashU)) showed relatively high and consistent accuracy across both outcomes.

The results further indicate that the highest performing assays have performance metrics that rival the gold standards of Aβ-PET and CSF.

If further validated, our findings will have significant impacts in diagnosis, screening and treatment for Alzheimer's dementia in the future.

Janelidze, Shorena,Bali, Divya,Ashton, Nicholas J,Barthélemy, Nicolas R,Vanbrabant, Jeroen,Stoops, Erik,Vanmechelen, Eugeen,He, Yingxin,Dolado, Anna Orduña,Triana-Baltzer, Gallen,Pontecorvo, Michael J,Zetterberg, Henrik,Kolb, Hartmuth,Vandijck, Manu,Blennow, Kaj,Bateman, Randall J,Hansson, Oskar, 2022, Head-to-head comparison of 10 plasma phospho-tau assays in prodromal Alzheimer’s disease, Oxford University Press

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