The aggregation of amyloid-beta (Abeta) peptide and its deposition in parts of the brain and cerebral vasculature form the central processes in the etiology of Alzheimer disease (AD) and cerebral amyloid angiopathy (CAA), respectively. Overwhelming evidence indicates low-molecular weight, soluble oligomers of Abeta (? 2 to 30mers) are the primary toxic agents inflicting synaptic dysfunction and eventually, neuronal death. However, how these toxic agents proliferate and induce widespread amyloid deposition throughout the brain, and what mechanism is involved in the amplification and propagation of toxic species are far from clear. Emerging evidence based on transgenic mice models suggest a transmissible nature of both endogenous and synthetic Abeta aggregates and implicate a prion-like mechanism of propagation in the dissemination and proliferation of toxic Abeta seeds. The pathogenic similarities between Abeta aggregates and mammalian prions do suggest that propagation may involve a conserved, template-assisted corruptive mechanism, by which specific oligomers gets replicated (and amplified) at the cost of fibril formation. Based on newly emerging data, it is increasingly being speculated that such prion-type transmissibility could be conserved across many amyloid diseases, but remains poorly understood. One of the main impediments for such an investigation has been the difficulty in isolating Abeta oligomers that are stable enough for biophysical analysis. Recently, we reported a self- propagating oligomer of Abeta42 (12-18mers) in vitro called Large Fatty Acid-derived Oligomers (LFAOs) (Kumar et al., 2012, J. Biol Chem), which is toxic to human neuroblastoma cells. Based on our preliminary data, we hypothesize that LFAOs are unique prion-like oligomers capable of cross-propagation by inducing 'corruptive propagation' to other homologous amyloidogenic proteins leading to biochemical similar toxic structures. In this project, we propose to use wild-type Abeta and specific CAA-linked mutant isoforms (Arctic, Dutch and Italian) to test our hypothesis and delineate fidelity of LFAO self-propagation (Aim 1) and the mechanism involved in cross-propagation (Aim 2), which form the basis for transmissibility. LFAOs, being the only biophysically well- characterized prion-like oligomers, present an ideal opportunity to investigate their molecular properties governing propagation. Mainly we will use in vitro biophysical methods to determine the mechanism and fidelity of propagation reactions, and to test how biophysical differences/similarities manifest in cellular functions by specific assays on both primary neuronal and primary endothelial cells. These investigations will lead to a profound understanding on the molecular aspects of transmissibility among Abeta aggregates, opening new perspectives in AD pathogenesis. In addition, this R15 proposal will provide significant inter-disciplinary research training opportunities for graduate and undergraduate students, which is an equally important objective of the proposed project.

Public Health Relevance

The proposed project is focused on a molecular understanding of how toxic agents responsible for Alzheimer's disease are able to spread to various areas of the brain. We hypothesize that a specific toxic protein aggregate isolated in our laboratory behaves as a toxic agent that can recruit healthy proteins to its own assembly and corrupt them to become toxic themselves, triggering a snowball effect. This kind of corruptive mechanism is well known to occur in diseases such as Mad Cow, and this project aims to probe into whether similar mechanism can occur in Alzheimer's disease and other related pathologies. We propose to identify the mechanism involved in the snowball effect leading to proliferation of toxicity. The implications of this work is far-reaching than just for AD pathology, as there are similarities between the toxic agents involved in AD and many other neurodegenerative diseases. This will also potentially open doors to new therapeutic interventions for the devastating neurological diseases of our time.

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Academic Research Enhancement Awards (AREA) (R15)
Project #
1R15AG046915-01A1
Application #
8812492
Study Section
Special Emphasis Panel (ZRG1-MDCN-R (86))
Program Officer
Yang, Austin Jyan-Yu
Project Start
2015-09-30
Project End
2018-08-31
Budget Start
2015-09-30
Budget End
2018-08-31
Support Year
1
Fiscal Year
2015
Total Cost
$368,479
Indirect Cost
$88,996
Name
University of Southern Mississippi
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
623335775
City
Hattiesburg
State
MS
Country
United States
Zip Code
39406
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Das, Pradipta K; Dean, Dexter N; Fogel, April L et al. (2017) Aqueous RAFT Synthesis of Glycopolymers for Determination of Saccharide Structure and Concentration Effects on Amyloid ? Aggregation. Biomacromolecules 18:3359-3366
Pate, Kayla M; Rogers, McCall; Reed, John Will et al. (2017) Anthoxanthin Polyphenols Attenuate A? Oligomer-induced Neuronal Responses Associated with Alzheimer's Disease. CNS Neurosci Ther 23:135-144
Rana, Pratip; Dean, Dexter N; Steen, Edward D et al. (2017) Fatty Acid Concentration and Phase Transitions Modulate A? Aggregation Pathways. Sci Rep 7:10370
Dean, Dexter N; Das, Pradipta K; Rana, Pratip et al. (2017) Strain-specific Fibril Propagation by an A? Dodecamer. Sci Rep 7:40787
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Ghag, Gaurav; Wolf, Lauren M; Reed, Randi G et al. (2016) Fully reduced granulin-B is intrinsically disordered and displays concentration-dependent dynamics. Protein Eng Des Sel 29:177-86