NMR Structure of the Human Prion Protein with the Pathological Q212P Mutation Reveals Unique Structural Features

Ilc, Gregor; Giachin, Gabriele; Jaremko, Mariusz; Jaremko, Łukasz; Benetti, Federico; Plavec, Janez; Zhukov, Igor; Legname, Giuseppe

doi:10.1371/journal.pone.0011715

Cited by 76 publications

(89 citation statements)

References 55 publications

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“…In a second example, mutation of prion protein Met-129 is an allelic risk factor for the development of neurodegenerative diseases, such as Alzheimer (39) as well as fatal familial insomnia and familial Creutzfield-Jacob (40). This Met residue in the wild type prion protein (PDB code 2kun) has three aromatic tyrosine residues within 10 Å, the closest at 5.5 Å separation (41). Another example, a known mutation of the RET proto-oncogene resulting in an M918T mutation within RET protein, is associated with the development of thyroid carcinoma (42,43), and Met-918 in the wild type structure (PDB code 2x2k) has six aromatic groups within 10 Å, with the nearest at 5.4 Å (44).…”

Section: Discussionmentioning

confidence: 99%

The Methionine-aromatic Motif Plays a Unique Role in Stabilizing Protein Structure

Valley

Cembran

Perlmutter

et al. 2012

Journal of Biological Chemistry

291

325

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Background:The interaction between methionine and aromatic residues in protein complexes is poorly understood. Results: The Met-aromatic motif is prevalent in known protein structures and stabilizes TNF ligand-receptor binding interactions. Conclusion:The Met sulfur-aromatic binding motif provides additional stabilization over purely hydrophobic interactions and at longer distances. Significance: This motif is prevalent and may be associated with a number of mutation-and age-associated diseases.

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Section: Discussionmentioning

confidence: 99%

The Methionine-aromatic Motif Plays a Unique Role in Stabilizing Protein Structure

Valley

Cembran

Perlmutter

et al. 2012

Journal of Biological Chemistry

291

325

View full text Add to dashboard Cite

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“…We have found one focus of prion protein structures is at the β2-α2 loop and its interacted Cterminal of H3 (Biljan et al, 2012a(Biljan et al, & 2012b(Biljan et al, & 2011Calzolai et al, 2000;Christen et al, 2009Christen et al, & 2012Damberger et al, 2011;Gossert et al, 2005;Ilc et al, 2010;Lee et al, 2010;Wen et al, 2010aWen et al, & 2010bKong et al, 2013;Perez et al, 2010Perez et al, & 2008Sweeting et al, 2013;Zahn et al, 2003;Zhang et al, 2000;Kurt et al, 2014aKurt et al, & 2014b. This article found there is a SB ASP177-ARG163 (O-N) in RaPrP C , which just keeps this loop being linked.…”

Section: Resultsmentioning

confidence: 91%

A review on the salt bridge ASP177-ARG163 (O–N) of wild-type rabbit prion protein

Zhang

Wang

2016

Journal of Biomolecular Structure and Dynamics

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Abstract:Prion diseases are invariably fatal and highly infectious neurodegenerative diseases that affect a wide variety of mammalian species such as sheep and goats, cattle, deer, elks, humans and mice etc., but rabbits have a low susceptibility to be infected by prion diseases with respect to other species. The stability of rabbit prion protein is due to its highly ordered β2-α2 loop (PLoS One 5(10) e13273 X-ray file of the rabbit prion protein, we can clearly observe this salt bridge. This article analyses the NMR and X-ray structures and gives an answer to the above question: the salt bridge presents at pH 6.5 in the X-ray structure is simply gone at pH 4.5 in the NMR structure is simply due to the different pH values that impact electrostatics at the salt bridge and hence also impact the structures. Moreover, some molecular dynamics simulation results of the X-ray structure are reported in this article to reveal the secrets of the structural stability of rabbit prion protein.

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“…PrP plaques were visible in both brain and the cerebellum but density of them was the lowest among all GSS families [135]. NMR structure of truncated peptide HuPrP (90-231) revealed different fold from that of the known structures of human PrP c [138]. In particular, α3 helix does not exhibit regular helical conformation in two residues 221…”

Section: The Codon 212 Pro 129 Met Mutationmentioning

confidence: 89%

Molecular Genetics of Gerstmann-Straussler-Scheinker Disease and Creutzfeld-Jakob Disease

Surewicz¹

2013

Hereditary Genetics

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Prion diseases are a group of transmissible neurodegenerative disorders associated with the misfolded form of the prion protein, PrP Sc . The latter isoform is derived by conformational conversion of the normal prion protein, PrP c . The gene encoding the prion protein is highly conserved among species. There are several distinct types of prion diseases in humans: kuru, Creutzfeldt -Jakob disease (CJD), Gerstmann-Sträussler-Scheinker disease (GSS) and Fatal Familial Insomnia (FFI) and its sporadic analogue, fatal sporadic insomnia. While human prion diseases are mostly sporadic, some 15% of CJD and all cases of GSS are hereditary disorders caused by mutations in the PRNP gene. There are two major types of mutations in PRNP: point mutations leading to amino acid substitutions and mutations leading to expansions of the octapeptide repeat region within the N-terminal part of the prion protein. This review describes different types of familial prion diseases linked to specific polymorphisms and mutation in PRNP.

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NMR Structure of the Human Prion Protein with the Pathological Q212P Mutation Reveals Unique Structural Features

Cited by 76 publications

References 55 publications

The Methionine-aromatic Motif Plays a Unique Role in Stabilizing Protein Structure

The Methionine-aromatic Motif Plays a Unique Role in Stabilizing Protein Structure

A review on the salt bridge ASP177-ARG163 (O–N) of wild-type rabbit prion protein

Molecular Genetics of Gerstmann-Straussler-Scheinker Disease and Creutzfeld-Jakob Disease

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