Prion Transmission Prevented by Modifying the β2-α2 Loop Structure of Host PrP<sup>C</sup>

Kurt, Timothy D.; Bett, Cyrus; Fernández‐Borges, Natalia; Joshi-Barr, Shivanjali; Hornemann, Simone; Rülicke, Thomas; Castilla, Joaquı́n; Wüthrich, Kurt; Aguzzi, Adriano; Sigurdson, Christina J.

doi:10.1523/jneurosci.4636-13.2014

Cited by 71 publications

(69 citation statements)

References 41 publications

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“…Indeed, β2-α2 loop substitutions were shown to impair prion conversion in vitro (25)(26)(27)(28) and in vivo, as transgenic mice that express PrP with 168R or with Y169G, S170N, and N174T substitutions resist infection with mouse-adapted prions (29,30). Collectively, these studies provide a rationale for investigating the role of the β2-α2 loop in barriers to human infection with CWD.…”

Section: Introductionmentioning

confidence: 94%

Human prion protein sequence elements impede cross-species chronic wasting disease transmission

et al. 2015

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Section: Introductionmentioning

confidence: 94%

Human prion protein sequence elements impede cross-species chronic wasting disease transmission

et al. 2015

Self Cite

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“…1). We paid particular attention to the loop region connecting the second strand of the β-sheet (β2) and α-helix 2 (the β2-α2 loop) because it is extremely well defined in elk PrP (8) and has been implicated in modulating interspecies prion transmission (9). In all three structures, residues 168-172 formed the previously reported, distinct 3 10 -helical turn (8).…”

Section: Significancementioning

confidence: 96%

Structural effects of PrP polymorphisms on intra- and interspecies prion transmission

Angers

Christiansen

Nalls

et al. 2014

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

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Understanding the molecular parameters governing prion propagation is crucial for controlling these lethal, proteinaceous, and infectious neurodegenerative diseases. To explore the effects of prion protein (PrP) sequence and structural variations on intra-and interspecies transmission, we integrated studies in deer, a species naturally susceptible to chronic wasting disease (CWD), a burgeoning, contagious epidemic of uncertain origin and zoonotic potential, with structural and transgenic (Tg) mouse modeling and cell-free prion amplification. CWD properties were faithfully maintained in deer following passage through Tg mice expressing cognate PrP, and the influences of naturally occurring PrP polymorphisms on CWD susceptibility were accurately reproduced in Tg mice or cellfree systems. Although Tg mice also recapitulated susceptibility of deer to sheep prions, polymorphisms that provided protection against CWD had distinct and varied influences. Whereas substitutions at residues 95 and 96 in the unstructured region affected CWD propagation, their protective effects were overridden during replication of sheep prions in Tg mice and, in the case of residue 96, deer. The inhibitory effects on sheep prions of glutamate at residue 226 in elk PrP, compared with glutamine in deer PrP, and the protective effects of the phenylalanine for serine substitution at the adjacent residue 225, coincided with structural rearrangements in the globular domain affecting interaction between α-helix 3 and the loop between β2 and α-helix 2. These structure-function analyses are consistent with previous structural investigations and confirm a role for plasticity of this tertiary structural epitope in the control of PrP conversion and strain propagation.protein structure | prion replication | protective polymorphisms | structural plasticity

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“…Specifically, Fab-P binds to a region that is affected by structural reorganization (residues 95-105), and thus may prevent the PrP C -to-PrP Sc transition. Our model of the recPrP-Fab-R1 complex identified an additional interaction site (residues 165-175) that is known to influence the misfolding of PrP (41)(42)(43); R1 binding to this site may inhibit misfolding of PrP.…”

Section: Introductionmentioning

confidence: 93%

Prion Protein—Antibody Complexes Characterized by Chromatography-Coupled Small-Angle X-Ray Scattering

Carter

Kim

Stroopinsky

et al. 2015

Biophysical Journal

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Aberrant self-assembly, induced by structural misfolding of the prion proteins, leads to a number of neurodegenerative disorders. In particular, misfolding of the mostly α-helical cellular prion protein (PrP(C)) into a β-sheet-rich disease-causing isoform (PrP(Sc)) is the key molecular event in the formation of PrP(Sc) aggregates. The molecular mechanisms underlying the PrP(C)-to-PrP(Sc) conversion and subsequent aggregation remain to be elucidated. However, in persistently prion-infected cell-culture models, it was shown that treatment with monoclonal antibodies against defined regions of the prion protein (PrP) led to the clearing of PrP(Sc) in cultured cells. To gain more insight into this process, we characterized PrP-antibody complexes in solution using a fast protein liquid chromatography coupled with small-angle x-ray scattering (FPLC-SAXS) procedure. High-quality SAXS data were collected for full-length recombinant mouse PrP [denoted recPrP(23-230)] and N-terminally truncated recPrP(89-230), as well as their complexes with each of two Fab fragments (HuM-P and HuM-R1), which recognize N- and C-terminal epitopes of PrP, respectively. In-line measurements by fast protein liquid chromatography coupled with SAXS minimized data artifacts caused by a non-monodispersed sample, allowing structural analysis of PrP alone and in complex with Fab antibodies. The resulting structural models suggest two mechanisms for how these Fabs may prevent the conversion of PrP(C) into PrP(Sc).

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Prion Transmission Prevented by Modifying the β2-α2 Loop Structure of Host PrP^C

Cited by 71 publications

References 41 publications

Human prion protein sequence elements impede cross-species chronic wasting disease transmission

Human prion protein sequence elements impede cross-species chronic wasting disease transmission

Structural effects of PrP polymorphisms on intra- and interspecies prion transmission

Prion Protein—Antibody Complexes Characterized by Chromatography-Coupled Small-Angle X-Ray Scattering

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Prion Transmission Prevented by Modifying the β2-α2 Loop Structure of Host PrPC

Cited by 71 publications

References 41 publications

Human prion protein sequence elements impede cross-species chronic wasting disease transmission

Human prion protein sequence elements impede cross-species chronic wasting disease transmission

Structural effects of PrP polymorphisms on intra- and interspecies prion transmission

Prion Protein—Antibody Complexes Characterized by Chromatography-Coupled Small-Angle X-Ray Scattering

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Product

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Prion Transmission Prevented by Modifying the β2-α2 Loop Structure of Host PrP^C