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Backbone NMR assignments of the C-terminal domain of the human prion protein and its disease‐associated T183A variant
by
De Simone, Alfonso
, Sanz-Hernández, Máximo
in
Creutzfeldt-Jakob disease
/ Experiments
/ Mutants
/ Mutation
/ Neurodegenerative diseases
/ NMR
/ Nuclear magnetic resonance
/ Prion protein
/ Protein folding
/ Proteins
/ Random coil
/ Transmissible spongiform encephalopathy
2021
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Backbone NMR assignments of the C-terminal domain of the human prion protein and its disease‐associated T183A variant
by
De Simone, Alfonso
, Sanz-Hernández, Máximo
in
Creutzfeldt-Jakob disease
/ Experiments
/ Mutants
/ Mutation
/ Neurodegenerative diseases
/ NMR
/ Nuclear magnetic resonance
/ Prion protein
/ Protein folding
/ Proteins
/ Random coil
/ Transmissible spongiform encephalopathy
2021
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Do you wish to request the book?
Backbone NMR assignments of the C-terminal domain of the human prion protein and its disease‐associated T183A variant
by
De Simone, Alfonso
, Sanz-Hernández, Máximo
in
Creutzfeldt-Jakob disease
/ Experiments
/ Mutants
/ Mutation
/ Neurodegenerative diseases
/ NMR
/ Nuclear magnetic resonance
/ Prion protein
/ Protein folding
/ Proteins
/ Random coil
/ Transmissible spongiform encephalopathy
2021
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Backbone NMR assignments of the C-terminal domain of the human prion protein and its disease‐associated T183A variant
Journal Article
Backbone NMR assignments of the C-terminal domain of the human prion protein and its disease‐associated T183A variant
2021
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Overview
Transmissible spongiform encephalopathies (TSEs) are fatal neurodegenerative disorders associated with the misfolding and aggregation of the human prion protein (huPrP). Despite efforts into investigating the process of huPrP aggregation, the mechanisms triggering its misfolding remain elusive. A number of TSE-associated mutations of huPrP have been identified, but their role at the onset and progression of prion diseases is unclear. Here we report the NMR assignments of the C-terminal globular domain of the wild type huPrP and the pathological mutant T183A. The differences in chemical shifts between the two variants reveal conformational alterations in some structural elements of the mutant, whereas the analyses of secondary shifts and random coil index provide indications on the putative mechanisms of misfolding of T183A huPrP.
Publisher
Springer Nature B.V
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