| Literature DB >> 25212850 |
Sarah K Fritschi1,2,3, Franziska Langer1,2, Stephan A Kaeser1,2, Luis F Maia1,2, Erik Portelius4, Dorothea Pinotsi5, Clemens F Kaminski5, David T Winkler6, Walter Maetzler1,2,7, Kathy Keyvani8, Philipp Spitzer9, Jens Wiltfang10, Gabriele S Kaminski Schierle5, Henrik Zetterberg4,11, Matthias Staufenbiel1,2, Mathias Jucker1,2.
Abstract
The soluble fraction of brain samples from patients with Alzheimer's disease contains highly biologically active amyloid-β seeds. In this study, we sought to assess the potency of soluble amyloid-β seeds derived from the brain and cerebrospinal fluid. Soluble Alzheimer's disease brain extracts were serially diluted and then injected into the hippocampus of young, APP transgenic mice. Eight months later, seeded amyloid-β deposition was evident even when the hippocampus received subattomole amounts of brain-derived amyloid-β. In contrast, cerebrospinal fluid from patients with Alzheimer's disease, which contained more than 10-fold higher levels of amyloid-β peptide than the most concentrated soluble brain extracts, did not induce detectable seeding activity in vivo. Similarly, cerebrospinal fluid from aged APP-transgenic donor mice failed to induce cerebral amyloid-β deposition. In comparison to the soluble brain fraction, cerebrospinal fluid largely lacked N-terminally truncated amyloid-β species and exhibited smaller amyloid-β-positive particles, features that may contribute to the lack of in vivo seeding by cerebrospinal fluid. Interestingly, the same cerebrospinal fluid showed at least some seeding activity in an in vitro assay. The present results indicate that the biological seeding activity of soluble amyloid-β species is orders of magnitude greater in brain extracts than in the cerebrospinal fluid.Entities:
Keywords: amyloid; biomarker; dementia; seeding
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Year: 2014 PMID: 25212850 PMCID: PMC5367518 DOI: 10.1093/brain/awu255
Source DB: PubMed Journal: Brain ISSN: 0006-8950 Impact factor: 13.501