Alzheimer's Disease Brain Organoids as a Source of Disease Relevant Amyloid-Beta Oligomers
Zanderigo, E. J.; Fatima, M.; Becker, S.; O'Neil, A. L.
Show abstract
Amyloid plaques are a hallmark of Alzheimers disease (AD) progression; however, the early stages of plaque formation and the specific amyloid-beta (A{beta}) species involved remain difficult to study. While post-mortem tissue provides insight into end-stage mature plaques, therapeutic development requires targeting the earliest A{beta} oligomers to arrest plaque formation. Furthermore, inherently toxic soluble A{beta} oligomers off-pathway from plaque formation are implicated as a driving force of AD pathology. It also remains unclear if the specific nature of key disease-relevant species can be accurately replicated in preparations of synthetic peptides.. To bridge this gap, we utilize brain organoids carrying AD mutations as a biologically authentic source for A{beta} peptides and oligomers. We demonstrate that these mutations do not disrupt organoid development and that the resulting conditioned media contains A{beta} oligomers with disease-relevant structures. Finally, we show that these oligomers can be concentrated and segregated via differential ultracentrifugation for further experimental applications.
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