Structural features distinguishing infectious ex vivo mammalian prions from non-infectious fibrillar assemblies generated in vitro

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Cassandra Terry
Robert L. Harniman
Jessica Sells
Adam Wenborn
Susan Joiner
Helen R. Saibil
Mervyn J. Miles
John Collinge
Jonathan D. F. Wadsworth
机构
[1] MRC Prion Unit at UCL,School of Chemistry
[2] UCL Institute of Prion Diseases,Institute of Structural and Molecular Biology, Department of Biological Sciences
[3] University of Bristol,School of Physics, H.H. Wills Physics Laboratory
[4] Birkbeck College,King’s Centre for Stem Cells & Regenerative Medicine
[5] University of London,undefined
[6] University of Bristol,undefined
[7] London Metropolitan University,undefined
[8] King’s College London,undefined
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Seeded polymerisation of proteins forming amyloid fibres and their spread in tissues has been implicated in the pathogenesis of multiple neurodegenerative diseases: so called “prion-like” mechanisms. While ex vivo mammalian prions, composed of multichain assemblies of misfolded host-encoded prion protein (PrP), act as lethal infectious agents, PrP amyloid fibrils produced in vitro generally do not. The high-resolution structure of authentic infectious prions and the structural basis of prion strain diversity remain unknown. Here we use cryo-electron microscopy and atomic force microscopy to examine the structure of highly infectious PrP rods isolated from mouse brain in comparison to non-infectious recombinant PrP fibrils generated in vitro. Non-infectious recombinant PrP fibrils are 10 nm wide single fibres, with a double helical repeating substructure displaying small variations in adhesive force interactions across their width. In contrast, infectious PrP rods are 20 nm wide and contain two fibres, each with a double helical repeating substructure, separated by a central gap of 8–10 nm in width. This gap contains an irregularly structured material whose adhesive force properties are strikingly different to that of the fibres, suggestive of a distinct composition. The structure of the infectious PrP rods, which cause lethal neurodegeneration, readily differentiates them from all other protein assemblies so far characterised in other neurodegenerative diseases.
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