Diffusible, highly bioactive oligomers represent a critical minority of soluble Aβ in Alzheimer’s disease brain

Hong, Wei; Wang, Zemin; Liu, Wen; O’Malley, Tiernan T.; Jin, Ming; Willem, Michael; Haass, Christian; Frosch, Matthew P.

doi:10.1007/s00401-018-1846-7

Cited by 113 publications

(148 citation statements)

References 64 publications

(124 reference statements)

Supporting

Mentioning

141

Contrasting

Order By: Relevance

“…The YZ1 iPSC line [95] was used to prepare neurogenin 2 (Ngn2)-induced human neurons [96] as described previously [41,45]. On iN day 4, cells were plated at 4000 cells/ well on Matrigel (Corning Life Sciences, Corning, NY)coated plates (#655090; Greiner Bio-One, Monroe, NC) and maintained until iN day 21, a time point when iNs are fully mature (Supplementary Figure 5A).…”

Section: Production Of Induced Neurons (Ins) From Human Induced Plurimentioning

confidence: 99%

“…Given the pleomorphic nature of Aβ assemblies formed in vitro [89] and those in extracts of human brain [25,41,92], it is reasonable to expect that toxicity is mediated by more than one Aβ assembly and that this could involve interactions between specific Aβ assemblies and specific receptors, such as PrP C and rather non-specific membrane perturbations [87]. PrP C is a membrane-associated protein best known for its role in transmissible spongiform encephalopathies [71].…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

PrP is a central player in toxicity mediated by soluble aggregates of neurodegeneration-causing proteins

et al. 2019

Self Cite

View full text Add to dashboard Cite

Neurodegenerative diseases are an enormous public health problem, affecting tens of millions of people worldwide. Nearly all of these diseases are characterized by oligomerization and fibrillization of neuronal proteins, and there is great interest in therapeutic targeting of these aggregates. Here, we show that soluble aggregates of α-synuclein and tau bind to plateimmobilized PrP in vitro and on mouse cortical neurons, and that this binding requires at least one of the same N-terminal sites at which soluble Aβ aggregates bind. Moreover, soluble aggregates of tau, α-synuclein and Aβ cause both functional (impairment of LTP) and structural (neuritic dystrophy) compromise and these deficits are absent when PrP is ablated, knocked-down, or when neurons are pre-treated with anti-PrP blocking antibodies. Using an all-human experimental paradigm involving: (1) isogenic iPSC-derived neurons expressing or lacking PRNP, and (2) aqueous extracts from brains of individuals who died with Alzheimer's disease, dementia with Lewy bodies, and Pick's disease, we demonstrate that Aβ, α-synuclein and tau are toxic to neurons in a manner that requires PrP C. These results indicate that PrP is likely to play an important role in a variety of late-life neurodegenerative diseases and that therapeutic targeting of PrP, rather than individual disease proteins, may have more benefit for conditions which involve the aggregation of more than one protein.

show abstract

Section: Production Of Induced Neurons (Ins) From Human Induced Plurimentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

PrP is a central player in toxicity mediated by soluble aggregates of neurodegeneration-causing proteins

et al. 2019

Self Cite

View full text Add to dashboard Cite

show abstract

“…Conversely, other work indicates that the large oligomer Aβ*56 induces specific changes in neuronal signaling leading to tau phosphorylation and aggregation, whereas dimers and trimers do not . Recent studies have shown that most Aβ extracted from AD brain is innocuous and only some species cause neurotoxicity . This suggests that generic antioligomer therapies, including Aβ antibodies, may be largely bound by the extensive pool of inactive oligomers, whereas targeting the small pool of diffusible, bioactive Aβ may be more useful.…”

Section: Evolution Of the Amyloid Cascade Hypothesismentioning

confidence: 99%

Amyloid‐β immunotherapy for alzheimer disease: Is it now a long shot?

Panza

Lozupone

Seripa

et al. 2019

Annals of Neurology

147

100

View full text Add to dashboard Cite

show abstract

“…While Aβ aggregation is widely acknowledged to be central to AD pathogenesis, an increasing body of evidence indicates that only a sub-population of Aβ aggregates are bioactive (Brinkmalm et al, 2018;Hong et al, 2018;Lesne, 2013). As with PrP and prion disease Sandberg et al, 2011;Sandberg et al, 2014), the form or forms of Aβ which mediate toxicity are not yet defined.…”

Section: Discussionmentioning

confidence: 99%

PrP-grafted antibodies bind certain amyloid β-protein aggregates, but do not prevent toxicity

et al. 2019

Self Cite

View full text Add to dashboard Cite

Background The prion protein (PrP) is known to bind certain soluble aggregates of the amyloid β-protein (Aβ), and two regions of PrP, one centered around residues 19-33, and the other around 87-112, are thought to be particularly important for this interaction. When either of these sequences are grafted into a human IgG the resulting antibodies react with disease-associated PrP conformers, whereas the parental b12 IgG does not.Methods Human antibodies containing grafts of PrP 19-33 or 87-112 were prepared as before (Solforosi et al. 2007) and tested for their ability to recognize synthetic and Alzheimer's disease (AD) brain-derived Aβ. Since aqueous extracts of AD brain contain a complex mixture of active and inactive Aβ species, we also assessed whether PrP-grafted antibodies could protect against neuritotoxicity mediated by AD brain-derived Aβ. For these experiments, human iPSC-derived neurons were grown in 96-well plates at 5000 cells per well and on post-induction day 21, AD brain extracts were added +/-test antibodies.Neurons were imaged for 3 days using an IncuCyte live-cell imaging system, and neurite number and density quantified. ResultsGrafted antibodies bound a significant portion of aggregated Aβ in aqueous AD extracts, but when these antibodies were co-incubated with neurons treated with brain extracts they did not reduce toxicity. By contrast, PrP and the PrP fragment N1 did protect against Aβ. ConclusionsThese results further demonstrate that not all Aβ oligomers are toxic and suggest that PrP derivatives may allow development of agents that differentially recognize toxic and innocuous Aβ aggregates.

show abstract

Diffusible, highly bioactive oligomers represent a critical minority of soluble Aβ in Alzheimer’s disease brain

Cited by 113 publications

References 64 publications

PrP is a central player in toxicity mediated by soluble aggregates of neurodegeneration-causing proteins

PrP is a central player in toxicity mediated by soluble aggregates of neurodegeneration-causing proteins

Amyloid‐β immunotherapy for alzheimer disease: Is it now a long shot?

PrP-grafted antibodies bind certain amyloid β-protein aggregates, but do not prevent toxicity

Contact Info

Product

Resources

About