- Petersen, Melissa E;
- Rafii, Michael S;
- Zhang, Fan;
- Hall, James;
- Julovich, David;
- Ances, Beau M;
- Schupf, Nicole;
- Krinsky-McHale, Sharon J;
- Mapstone, Mark;
- Silverman, Wayne;
- Lott, Ira;
- Klunk, William;
- Head, Elizabeth;
- Christian, Brad;
- Foroud, Tatiana;
- Lai, Florence;
- Rosas, H Diana;
- Zaman, Shahid;
- Wang, Mei-Cheng;
- Tycko, Benjamin;
- Lee, Joseph H;
- Handen, Benjamin;
- Hartley, Sigan;
- Fortea, Juan;
- O’Bryant, Sid;
- Syndrome, for the Alzheimer’s Biomarker Consortium–Down
Background
The need for diagnostic biomarkers of cognitive decline is particularly important among aging adults with Down syndrome (DS). Growing empirical support has identified the utility of plasma derived biomarkers among neurotypical adults with mild cognitive impairment (MCI) and Alzheimer's disease (AD); however, the application of such biomarkers has been limited among the DS population.Objective
This study aimed to investigate the cross-sectional diagnostic performance of plasma neurofilament light chain (Nf-L) and total-tau, individually and in combination among a cohort of DS adults.Methods
Plasma samples were analyzed from n = 305 (n = 225 cognitively stable (CS); n = 44 MCI-DS; n = 36 DS-AD) participants enrolled in the Alzheimer's Biomarker Consortium -Down Syndrome.Results
In distinguishing DS-AD participants from CS, Nf-L alone produced an AUC of 90%, total-tau alone reached 74%, and combined reached an AUC of 86%. When age and gender were included, AUC increased to 93%. Higher values of Nf-L, total-tau, and age were all shown to be associated with increased risk for DS-AD. When distinguishing MCI-DS participants from CS, Nf-L alone produced an AUC of 65%, while total-tau alone reached 56%. A combined model with Nf-L, total-tau, age, and gender produced an AUC of 87%. Both higher values in age and total-tau were found to increase risk for MCI-DS; Nf-L levels were not associated with increased risk for MCI-DS.Conclusion
Advanced assay techniques make total-tau and particularly Nf-L useful biomarkers of both AD pathology and clinical status in DS and have the potential to serve as outcome measures in clinical trials for future disease-modifying drugs.