Alzheimer’s Amyloid-β Oligomers Rescue Cellular Prion Protein Induced Tau Reduction via the Fyn Pathway

Chen, Rong-Jie; Chang, Wei-Wei; Lin, Yu‐Chun; Cheng, Pei‐Lin; Chen, Yun‐Ru

doi:10.1021/cn400085q

Cited by 27 publications

(25 citation statements)

References 41 publications

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“…This reinforces previously reported microarray data in N2a cells [65] and PrP C mutant mice at younger stages compared with adults (2-3 months) [72][73][74]. However, these observations are partially in contrast with some recently published results, using human neuroblastoma [75] and HEK293 cells [74]. In these studies, forced PrP C expression in transfected cells with low expression levels of endogenous PrP C decreased total tau protein levels [75].…”

Section: Discussionsupporting

confidence: 91%

“…However, these observations are partially in contrast with some recently published results, using human neuroblastoma [75] and HEK293 cells [74]. In these studies, forced PrP C expression in transfected cells with low expression levels of endogenous PrP C decreased total tau protein levels [75].…”

Section: Discussioncontrasting

confidence: 66%

“…In fact, it has been proposed that PrP C suppresses tau transcription, probably though modulation of the Fyn pathway [75]. However when we crossed APP/PS1 mice with a mouse model of tau overexpression under a -actin promoter, reduction of PrP C levels by siRNA induced increased presence of both endogenous (regulated by tau promoter) and exogenous tau-GFP (regulated by -actin promoter) (Fig.…”

Section: Prp C Expression Addls Tau Phosphorylation and Neuroprotecmentioning

confidence: 91%

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Role of PrPC Expression in Tau Protein Levels and Phosphorylation in Alzheimer’s Disease Evolution

et al. 2014

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Alzheimer's disease (AD) is characterized by the presence of amyloid plaques mainly consisting of hydrophobic -amyloid peptide (A) aggregates and neurofibrillary tangles (NFTs) composed principally of hyperphosphorylated tau. A oligomers have been described as the earliest effectors to negatively affect synaptic structure and plasticity in the affected brains, and cellular prion protein (PrP C ) has been proposed as receptor for these oligomers.The most widely accepted theory holds that the toxic effects of A are upstream of change in tau, a neuronal microtubule-associated protein that promotes the polymerization and stabilization of microtubules. However, tau is considered decisive for the progression of neurodegeneration, and indeed tau pathology correlates well with clinical symptoms such as dementia. Different pathways can lead to abnormal phosphorylation, and, as a consequence, tau aggregates into Paired Helical Filaments (PHF) and later on into NFTs.Reported data suggest a regulatory tendency of PrP C expression in the development of AD, and a putative relationship between PrP C and tau processing is emerging. However the role of tau/PrP C interaction in AD is poorly understood.In this study we show increased susceptibility to A derived diffusible ligands (ADDLs) in neuronal primary cultures from PrP C knock-out mice, compared to wild-type, which correlates with increased tau expression. Moreover, we found increased PrP C expression that paralleled with tau at early ages in an AD murine model, and in early Braak stages of AD in affected individuals. Taken together, these results suggest a protective role for PrP C in AD by down-regulating tau expression, and they point to this protein as being crucial in the molecular events that lead to neurodegeneration in AD.

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Section: Discussionsupporting

confidence: 91%

Section: Discussioncontrasting

confidence: 66%

Section: Prp C Expression Addls Tau Phosphorylation and Neuroprotecmentioning

confidence: 91%

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Role of PrPC Expression in Tau Protein Levels and Phosphorylation in Alzheimer’s Disease Evolution

et al. 2014

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“…Phosphorylated Fyn level increased in a dose-dependent manner 2 hours after Aβ oligomer treatment and interestingly it became decreased 1 day after this treatment. Surprisingly, the murine PrP c M128V, which correspond with the high AD risk polymorphic human PrP c M129V [74] allele was able to bind Aβ oligomers, but it was unable to reverse the tau reduction [13]. This may be another explanation why this polymorphism was associated with lower IQ and white matter reduction in the study mentioned earlier in this article.…”

Section: Cooperation?mentioning

confidence: 58%

“…[13,47], and also Lar son and Lesne [48]) suggest that confounding results about PrP c -mediated impairments, as those described previously, may be attributed only to a subset of Aβ oligomers that are mediated through PrP c . For example, no dependence in LTP impairments in studies of Calella et al [11] may be a result of low levels of Aβ dimers in young aged Tg-mice.…”

Section: Cooperation?mentioning

confidence: 83%

New light on prions: putative role of co-operation of PrPc and Aβ proteins in cognition

Chrobak¹,

Adamek²

2014

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Aβ-induced acceleration of Alzheimer-related τ-pathology spreading and its association with prion protein

et al. 2019

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Alzheimer’s Amyloid-β Oligomers Rescue Cellular Prion Protein Induced Tau Reduction via the Fyn Pathway

Cited by 27 publications

References 41 publications

Role of PrPC Expression in Tau Protein Levels and Phosphorylation in Alzheimer’s Disease Evolution

Role of PrPC Expression in Tau Protein Levels and Phosphorylation in Alzheimer’s Disease Evolution

New light on prions: putative role of co-operation of PrPc and Aβ proteins in cognition

Aβ-induced acceleration of Alzheimer-related τ-pathology spreading and its association with prion protein

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