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Abstract / Description of output
Mammalian prions are unusual infectious agents, as they are thought to consist solely of aggregates of misfolded prion protein (PrP). Generation of synthetic prions, composed of recombinant PrP (recPrP) refolded into fibrils, has been utilised to address whether PrP aggregates are indeed infectious prions. In several reports, neurological disease similar to transmissible spongiform encephalopathy (TSE) has been described following inoculation and passage of various forms of fibrils in transgenic mice and hamsters. However in studies described here we show that inoculation of recPrP fibrils does not cause TSE disease, but instead seeds the formation of PrP amyloid plaques in PrP-P101L knock-in transgenic mice (101LL). Importantly, both WT-recPrP fibrils and 101L-recPrP fibrils can seed plaque formation, indicating the fibrillar conformation and not the primary sequence of PrP in the inoculum is important in initiating seeding. No replication of infectious prions or TSE disease was observed following both primary inoculation and subsequent subpassage. These data therefore argue against recPrP fibrils being infectious prions and instead indicate that these pre-formed seeds are acting to accelerate the formation of PrP amyloid plaques in 101LL Tg mice. Additionally, these data reproduce a phenotype which was previously observed in 101LL mice following inoculation with brain extract containing in vivo generated PrP amyloid fibrils, which has not been shown for other synthetic prion models.
These data are reminiscent of the “prion-like” spread of aggregated forms of the beta-amyloid peptide (Aβ), α-synuclein and tau observed following inoculation of transgenic mice with pre-formed seeds of each misfolded protein. Hence, even when the protein is PrP, misfolding and aggregation do not reproduce the full clinicopathological phenotype of disease. The initiation and spread of protein aggregation in transgenic mouse lines following inoculation with pre-formed fibrils may therefore more closely resemble a seeded proteinopathy than an infectious TSE disease.
These data are reminiscent of the “prion-like” spread of aggregated forms of the beta-amyloid peptide (Aβ), α-synuclein and tau observed following inoculation of transgenic mice with pre-formed seeds of each misfolded protein. Hence, even when the protein is PrP, misfolding and aggregation do not reproduce the full clinicopathological phenotype of disease. The initiation and spread of protein aggregation in transgenic mouse lines following inoculation with pre-formed fibrils may therefore more closely resemble a seeded proteinopathy than an infectious TSE disease.
Original language | English |
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Pages (from-to) | 611-624 |
Journal | Acta Neuropathologica |
Volume | 132 |
Issue number | 4 |
Early online date | 4 Jul 2016 |
DOIs | |
Publication status | Published - Oct 2016 |
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Dive into the research topics of 'PrP aggregation can be seeded by pre-formed recombinant PrP amyloid fibrils without the replication of infectious prions'. Together they form a unique fingerprint.Projects
- 2 Finished
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Livestock neurobiology
Gill, A., Barron, R., Beard, P., Brunton, P., Goldmann, W., Hume, D., Hunter, N., Lawrence, A., Mabbott, N., Manson, J., McColl, B., Meddle, S. & Wishart, T.
1/04/12 → 31/03/17
Project: Research
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Accumulation of PrP amyloid in vivo that is not infectious
Barron, R.
1/05/08 → 28/02/11
Project: Research