Distinct synthetic Aβ prion strains producing different amyloid deposits in bigenic mice

Stöhr, Jan; Condello, Carlo; Watts, Joel C.; Bloch, Lillian; Oehler, Abby; Nick, Mimi; DeArmond, Stephen J.; Giles, Kurt; DeGrado, William F.; Prusiner, Stanley B.

doi:10.1073/pnas.1408968111

Cited by 153 publications

(169 citation statements)

References 43 publications

Supporting

Mentioning

158

Contrasting

Unclassified

Order By: Relevance

“…46 Similar strain propagation of amyloid-β has been demonstrated with synthetic peptides, and suggested as basis for phenotypic variability to human AD. 47,48 These data taken together make a sophisticated case for spreading toxicity in a prion-like manner.…”

Section: Cte As a Prion Diseasementioning

confidence: 99%

Chronic traumatic encephalopathy: A paradigm in search of evidence?

Castellani

2015

Laboratory Investigation

View full text Add to dashboard Cite

Chronic traumatic encephalopathy (CTE) has been in the medical literature since the 1920s. It is characterized clinically by diverse neuropsychiatric symptoms, and pathologically by variable degrees of phosphorylated tau accumulation in the brain. The evolving paradigm for the pathogenesis of CTE suggests that concussion or subconcussion from athletic participation initiates a cascade of pathologic events, encompassing neuroinflammation and protein templating with trans-synaptic neurotoxicity. The end result is neurologic and neurobehavioral deterioration, often with self-harm. Although these concepts warrant further investigation, the available evidence permits no conclusions as regards the pathogenesis of the reported findings. Investigations into the role of premorbid or co-morbid neurodegenerative diseases has been limited to date, and in-depth genetic analyses have not been performed. The role of concussion or subconcussion if any, whether and how the condition progresses over time, the extent of phosphorylated tau in clinically normal athletes, the role of phosphorylated tau as a toxic species versus an inert disease response, and whether protein templating has any in vivo relevance remain to be elucidated.

show abstract

Section: Cte As a Prion Diseasementioning

confidence: 99%

Chronic traumatic encephalopathy: A paradigm in search of evidence?

Castellani

2015

Laboratory Investigation

View full text Add to dashboard Cite

show abstract

“…Furthermore, Aβ40 forms small dimers (two monomers) and tetramers (four monomers) and, when injected into mouse brains, long straight fibrils. 9,10 Aβ42 can also form larger assemblies, including hexamers (six monomers) and dodecamers (12 monomers). 9 But Aβ42 fibrils were shorter and the plaques smaller and more numerous when injected into mice.…”

Section: Molecular Origamimentioning

confidence: 99%

“…9 But Aβ42 fibrils were shorter and the plaques smaller and more numerous when injected into mice. 10 Even the same Aβ subtype can form different shapes, which seem to influence clinical presentations. A recent study examined brain tissue from two patients with sporadic AD, both of whom expressed Aβ40.…”

Section: Molecular Origamimentioning

confidence: 99%

The link between laughing death and Alzheimer's disease

Greener¹

2014

Prog. Neurol. Psychiatry

View full text Add to dashboard Cite

show abstract

“…Moreover, PrP prions occur in multiple "strains," which differ in their PrP Sc conformations as well as their biochemical properties and neuropathological lesions (Bessen and Marsh, 1994;Telling et al, 1996;Collinge and Clarke, 2007). The phenomenon of strains is not limited to PrP prions and has recently been recognized in the more common NDs, both in synthetic preparations (Frost et al, 2009;Guo et al, 2013;Stöhr et al, 2014) and in brains from patients (Clavaguera et al, 2013;Lu et al, 2013b;Watts et al, 2013Watts et al, , 2014Sanders et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

Different 2-Aminothiazole Therapeutics Produce Distinct Patterns of Scrapie Prion Neuropathology in Mouse Brains

Giles

Berry

Condello

et al. 2015

J Pharmacol Exp Ther

Self Cite

View full text Add to dashboard Cite

Because no drug exists that halts or even slows any neurodegenerative disease, developing effective therapeutics for any prion disorder is urgent. We recently reported two compounds (IND24 and IND81) with the 2-aminothiazole (2-AMT) chemical scaffold that almost doubled the incubation times in scrapie prion-infected, wild-type (wt) FVB mice when given in a liquid diet. Remarkably, oral prophylactic treatment with IND24 beginning 14 days prior to intracerebral prion inoculation extended survival from ∼120 days to over 450 days. In addition to IND24, we evaluated the pharmacokinetics and efficacy of five additional 2-AMTs; one was not followed further because its brain penetration was poor. Of the remaining four new 2-AMTs, IND114338 doubled and IND125 tripled the incubation times of RML-inoculated wt and Tg4053 mice overexpressing wt mouse prion protein (PrP), respectively. Neuropathological examination of the brains from untreated controls showed a widespread deposition of self-propagating, b-sheet-rich "scrapie" isoform (PrP Sc ) prions accompanied by a profound astrocytic gliosis. In contrast, mice treated with 2-AMTs had lower levels of PrP Sc and associated astrocytic gliosis, with each compound resulting in a distinct pattern of deposition. Notably, IND125 prevented both PrP Sc accumulation and astrocytic gliosis in the cerebrum. Progressive central nervous system dysfunction in the IND125-treated mice was presumably due to the PrP Sc that accumulated in their brainstems. Disappointingly, none of the four new 2-AMTs prolonged the lives of mice expressing a chimeric human/ mouse PrP transgene inoculated with Creutzfeldt-Jakob disease prions.

show abstract

Distinct synthetic Aβ prion strains producing different amyloid deposits in bigenic mice

Cited by 153 publications

References 43 publications

Chronic traumatic encephalopathy: A paradigm in search of evidence?

Chronic traumatic encephalopathy: A paradigm in search of evidence?

The link between laughing death and Alzheimer's disease

Different 2-Aminothiazole Therapeutics Produce Distinct Patterns of Scrapie Prion Neuropathology in Mouse Brains

Contact Info

Product

Resources

About