Exosomal Biomarkers in Down Syndrome and Alzheimer's Disease

Authors

Eric D. Hamlett, University of Denver, Medical University of South Carolina
Aurélie Ledreux, University of DenverFollow
Huntington Potter, University of Colorado Anschutz Medical Campus
Heidi J. Chial, University of Colorado Anschutz Medical Campus
David Patterson, University of DenverFollow
Joaquin M. Espinosa, University of Colorado Anschutz Medical Campus
Brianne M. Bettcher, University of Colorado Anschutz Medical Campus
Ann‐Charlotte Granholm, University of DenverFollow

Publication Date

9-5-2017

Document Type

Article

Organizational Units

Knoebel Institute for Healthy Aging

Keywords

Down syndrome, Alzheimer's disease, Neurodegeneration, Exosomes, Neuroinflammation, Oxidative stress

Abstract

Every person with Down syndrome (DS) has the characteristic features of Alzheimer's disease (AD) neuropathology in their brain by the age of forty, and most go on to develop AD dementia. Since people with DS show highly variable levels of baseline function, it is often difficult to identify early signs of dementia in this population. The discovery of blood biomarkers predictive of dementia onset and/or progression in DS is critical for developing effective clinical diagnostics. Our recent studies show that neuron-derived exosomes, which are small extracellular vesicles secreted by most cells in the body, contain elevated levels of amyloid-beta peptides and phosphorylated-Tau that could indicate a preclinical AD phase in people with DS starting in childhood. We also found that the relative levels of these biomarkers were altered following dementia onset. Exosome release and signaling are dependent on cellular redox homeostasis as well as on inflammatory processes, and exosomes may be involved in the immune response, suggesting a dual role as both triggers of inflammation in the brain and propagators of inflammatory signals between brain regions. Based on recently reported connections between inflammatory processes and exosome release, the elevated neuroinflammatory state observed in people with DS may affect exosomal AD biomarkers. Herein, we discuss findings from studies of people with DS, people with DS and AD (DS-AD), and mouse models of DS showing new connections between neuroinflammatory pathways, oxidative stress, exosomes, and exosome-mediated signaling, which may inform future AD diagnostics, preventions, and treatments in the DS population as well as in the general population.

Publication Statement

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Recommended Citation

Hamlett, Eric D, Ledreux, Aurélie, Potter, Huntington, Chial, Heidi J, Patterson, David, Espinosa, Joaquin M, . . . Granholm, Ann-Charlotte. (2018). Exosomal biomarkers in Down syndrome and Alzheimer's disease. Free Radical Biology & Medicine, 114, 110-121. doi: 10.1016/j.freeradbiomed.2017.08.028.