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• W2014668312 endingPage "2403" @default.
• W2014668312 startingPage "2393" @default.
• W2014668312 abstract "Amyloid aggregates of a C-truncated Y145Stop mutant of human prion protein, huPrP23-144, associated with a heritable amyloid angiopathy, have previously been shown to contain a compact, relatively rigid, and beta-sheet-rich approximately 30-residue amyloid core near the C-terminus under physiologically relevant conditions. In contrast, the remaining huPrP23-144 residues display considerable conformational dynamics, as evidenced by the absence of corresponding signals in cross-polarization (CP)-based solid-state NMR (SSNMR) spectra under ambient conditions and their emergence in analogous spectra recorded at low temperature on frozen fibril samples. Here, we present the direct observation of residues comprising the flexible N-terminal domain of huPrP23-144 amyloid by using 2D J-coupling-based magic-angle spinning (MAS) SSNMR techniques. Chemical shifts for these residues indicate that the N-terminal domain is effectively an ensemble of protein chains with random-coil-like conformations. Interestingly, a detailed analysis of signal intensities in CP-based 3D SSNMR spectra suggests that non-negligible molecular motions may also be occurring on the NMR time scale within the relatively rigid core of huPrP23-144 amyloid. To further investigate this hypothesis, quantitative measurements of backbone dipolar order parameters and transverse spin relaxation rates were performed for the core residues. The observed order parameters indicate that, on the submicrosecond time scale, these residues are effectively rigid and experience only highly restricted and relatively uniform motions similar to those characteristic for well-structured regions of microcrystalline proteins. On the other hand, significant variations in magnitude of transverse spin relaxation rates were noted for residues present at different locations within the core region and correlated with observed differences in spectral intensities. While interpreted only qualitatively at the present time, the extent of the observed variations in transverse relaxation rates is consistent with the presence of relatively slow, microsecond-millisecond time scale chemical exchange type phenomena within the huPrP23-144 amyloid core." @default.
• W2014668312 created "2016-06-24" @default.
• W2014668312 creator A5002874878 @default.
• W2014668312 creator A5039607513 @default.
• W2014668312 creator A5046490885 @default.
• W2014668312 creator A5080398993 @default.
• W2014668312 date "2010-02-01" @default.
• W2014668312 modified "2023-09-27" @default.
• W2014668312 title "Conformational Flexibility of Y145Stop Human Prion Protein Amyloid Fibrils Probed by Solid-State Nuclear Magnetic Resonance Spectroscopy" @default.
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• W2014668312 doi "https://doi.org/10.1021/ja909827v" @default.
• W2014668312 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/2838504" @default.
• W2014668312 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/20121096" @default.
• W2014668312 hasPublicationYear "2010" @default.
• W2014668312 type Work @default.
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