β-Sheet core of human prion protein amyloid fibrils as determined by hydrogen/deuterium exchange

Lu, Xiaojun; Wintrode, Patrick L.; Surewicz, Witold K.

doi:10.1073/pnas.0608447104

Cited by 212 publications

(296 citation statements)

References 48 publications

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“…Consistent with the established increase in ␤-structure content upon conversion to amyloid (20,29), the only scenario compatible with the present data is that residues within this "core" region stack as single molecule layers with close proximity of same residues in the adjacent PrP molecules. The location of this tightly packed ␤-sheet region correlates remarkably well with recent H/D exchange studies conducted in our laboratory (19), which mapped an exchangeprotected core to residues Ϸ169-221.…”

Section: Resultssupporting

confidence: 65%

“…This critical gap in TSE research largely reflects experimental difficulties in structural studies of large protein aggregates such as amyloid fibrils. Our recent hydrogen/ deuterium (H/D) exchange study has provided an initial lowresolution insight into the location of the ␤-sheet core in the recombinant PrP amyloid (19). However, the molecular architecture of this core region remains unknown.…”

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confidence: 99%

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Molecular architecture of human prion protein amyloid: A parallel, in-register β-structure

Cobb

Sönnichsen

Mchaourab³

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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Transmissible spongiform encephalopathies (TSEs) represent a group of fatal neurodegenerative diseases that are associated with conformational conversion of the normally monomeric and ␣-helical prion protein, PrP C , to the ␤-sheet-rich PrP Sc . This latter conformer is believed to constitute the main component of the infectious TSE agent. In contrast to high-resolution data for the PrP C monomer, structures of the pathogenic PrP Sc or synthetic PrP Sc -like aggregates remain elusive. Here we have used sitedirected spin labeling and EPR spectroscopy to probe the molecular architecture of the recombinant PrP amyloid, a misfolded form recently reported to induce transmissible disease in mice overexpressing an N-terminally truncated form of PrP C . Our data show that, in contrast to earlier, largely theoretical models, the conformational conversion of PrP C involves major refolding of the C-terminal ␣-helical region. The core of the amyloid maps to C-terminal residues from Ϸ160 -220, and these residues form single-molecule layers that stack on top of one another with parallel, in-register alignment of ␤-strands. This structural insight has important implications for understanding the molecular basis of prion propagation, as well as hereditary prion diseases, most of which are associated with point mutations in the region found to undergo a refolding to ␤-structure.EPR ͉ spin labeling ͉ transmissible spongiform encephalopathy

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Section: Resultssupporting

confidence: 65%

mentioning

confidence: 99%

Molecular architecture of human prion protein amyloid: A parallel, in-register β-structure

Cobb

Sönnichsen

Mchaourab³

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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303

342

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“…24,25 Instead, a variety of studies have investigated the structure of amyloid fibrils produced in vitro from recombinant PrP. [26][27][28][29][30][31][32][33][34][35] Hereditary prion diseases include C-terminally truncated variants of the PrP, Y145X, Q160X, Y226X, and Q227X. Previously, we showed that the b-sheet content is highly similar in amyloid fibrils of the Y145X and Q160X stop mutants of human PrP.…”

Section: Resultsmentioning

confidence: 99%

Determination of amyloid core structure using chemical shifts

Skora

Zweckstetter

2012

Protein Science

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Amyloid fibrils are the pathological hallmark of a large variety of neurodegenerative disorders. The structural characterization of amyloid fibrils, however, is challenging due to their non-crystalline, heterogeneous, and often dynamic nature. Thus, the structure of amyloid fibrils of many proteins is still unknown. We here show that the structure calculation program CS-Rosetta can be used to obtain insight into the core structure of amyloid fibrils. Driven by experimental solid-state NMR chemical shifts and taking into account the polymeric nature of fibrils CS-Rosetta allows modeling of the core of amyloid fibrils. Application to the Y145X stop mutant of the human prion protein reveals a left-handed b-helix.

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“…[10][11][12] There has been some recent progress in defining the molecular architecture of prion amyloid fibers. 13,14 The mammalian prion proteins have a high homology at the sequence and structural level. All mammalian PrP C studied consist of two structurally distinct domains.…”

Section: Introductionmentioning

confidence: 99%

Dynamics of a truncated prion protein, PrP(113–231), from ¹⁵N NMR relaxation: Order parameters calculated and slow conformational fluctuations localized to a distinct region

et al. 2009

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Prion diseases are associated with the misfolding of the prion protein (PrP C ) from a largely a-helical isoform to a b-sheet rich oligomer (PrP Sc ). Flexibility of the polypeptide could contribute to the ability of PrP C to undergo the conformational rearrangement during PrP C -PrP Sc interactions, which then leads to the misfolded isoform. We have therefore examined the molecular motions of mouse PrP C , residues 113-231, in solution, using 15 N NMR relaxation measurements. A truncated fragment has been used to eliminate the effect of the 90-residue unstructured tail of PrP C so the dynamics of the structured domain can be studied in isolation. 15 N longitudinal (T 1 ) and transverse relaxation (T 2 ) times as well as the proton-nitrogen nuclear Overhauser effects have been used to calculate the spectral density at three frequencies, 0, x N, and 0.87x H . Spectral densities at each residue indicate various time-scale motions of the main-chain. Even within the structured domain of PrP C , a diverse range of motions are observed. We find that removal of the tail increases T 2 relaxation times significantly indicating that the tail is responsible for shortening of T 2 times in full-length PrP C . The truncated fragment of PrP has facilitated the determination of meaningful order parameters (S 2 ) from the relaxation data and shows for the first time that all three helices in PrP C have similar rigidity. Slow conformational fluctuations of mouse PrP C are localized to a distinct region that involves residues 171 and 172. Interestingly, residues 170-175 have been identified as a segment within PrP that will form a steric zipper, believed to be the fundamental amyloid unit. The flexibility within these residues could facilitate the PrP C -PrP Sc recognition process during fibril elongation.

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β-Sheet core of human prion protein amyloid fibrils as determined by hydrogen/deuterium exchange

Cited by 212 publications

References 48 publications

Molecular architecture of human prion protein amyloid: A parallel, in-register β-structure

Molecular architecture of human prion protein amyloid: A parallel, in-register β-structure

Determination of amyloid core structure using chemical shifts

Dynamics of a truncated prion protein, PrP(113–231), from ¹⁵N NMR relaxation: Order parameters calculated and slow conformational fluctuations localized to a distinct region

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β-Sheet core of human prion protein amyloid fibrils as determined by hydrogen/deuterium exchange

Cited by 212 publications

References 48 publications

Molecular architecture of human prion protein amyloid: A parallel, in-register β-structure

Molecular architecture of human prion protein amyloid: A parallel, in-register β-structure

Determination of amyloid core structure using chemical shifts

Dynamics of a truncated prion protein, PrP(113–231), from 15N NMR relaxation: Order parameters calculated and slow conformational fluctuations localized to a distinct region

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Dynamics of a truncated prion protein, PrP(113–231), from ¹⁵N NMR relaxation: Order parameters calculated and slow conformational fluctuations localized to a distinct region