Blood protein predictors of brain amyloid for enrichment in clinical trials?

AIBL Research Group; Ashton, Nicholas J; Ashton, Nicholas J; Baird, Alison L; Baker, David; Bazenet, Chantal; Covin, Antonia; Dobson, Richard J; Graf, John; Hehir, Cristina Tan; Hye, Abdul; Kiddle, Steven J; Lovestone, Simon; Miller, Bruce L; Rabinovici, Gil D; Rosen, Howard J; Thurfjell, Lennart; Torres, Andrew; Ward, Malcolm; Westwood, Sarah; Wong, Karyuan Vivian; Zhang, Zhanpan

Blood protein predictors of brain amyloid for enrichment in clinical trials?

Authors: AIBL Research Group
Nicholas J Ashton
Nicholas J Ashton
Alison L Baird
David Baker
Chantal Bazenet
Antonia Covin
Richard J Dobson
John Graf
Cristina Tan Hehir
Abdul Hye
Steven J Kiddle
Simon Lovestone
Bruce L Miller
Gil D Rabinovici
Howard J Rosen
Lennart Thurfjell
Andrew Torres
Malcolm Ward
Sarah Westwood
Karyuan Vivian Wong
Zhanpan Zhang
Publication date: 1 March 2015
Publisher: Alzheimers Dement (Amst)
Doi

Abstract

BACKGROUND: Measures of neocortical amyloid burden (NAB) identify individuals who are at substantially greater risk of developing Alzheimer's disease (AD). Blood-based biomarkers predicting NAB would have great utility for the enrichment of AD clinical trials, including large-scale prevention trials. METHODS: Nontargeted proteomic discovery was applied to 78 subjects from the Australian Imaging, Biomarkers and Lifestyle Flagship Study of Ageing with a range of NAB values. Technical and independent replications were performed by immunoassay. RESULTS: Seventeen discovery candidates were selected for technical replication. α2-Macroglobulin, fibrinogen γ-chain (FGG), and complement factor H-related protein 1 were confirmed to be associated with NAB. In an independent cohort, FGG plasma levels combined with age predicted NAB had a sensitivity of 59% and specificity of 78%. CONCLUSION: A single blood protein, FGG, combined with age, was shown to relate to NAB and therefore could have potential for enrichment of clinical trial populations