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Complex folding and misfolding effects of deer-specific amino acid substitutions in the ?2-?2 loop of murine prion protein.


ABSTRACT: The ?2-?2 loop of PrP(C) is a key modulator of disease-associated prion protein misfolding. Amino acids that differentiate mouse (Ser169, Asn173) and deer (Asn169, Thr173) PrP(C) appear to confer dramatically different structural properties in this region and it has been suggested that amino acid sequences associated with structural rigidity of the loop also confer susceptibility to prion disease. Using mouse recombinant PrP, we show that mutating residue 173 from Asn to Thr alters protein stability and misfolding only subtly, whilst changing Ser to Asn at codon 169 causes instability in the protein, promotes oligomer formation and dramatically potentiates fibril formation. The doubly mutated protein exhibits more complex folding and misfolding behaviour than either single mutant, suggestive of differential effects of the ?2-?2 loop sequence on both protein stability and on specific misfolding pathways. Molecular dynamics simulation of protein structure suggests a key role for the solvent accessibility of Tyr168 in promoting molecular interactions that may lead to prion protein misfolding. Thus, we conclude that 'rigidity' in the ?2-?2 loop region of the normal conformer of PrP has less effect on misfolding than other sequence-related effects in this region.

SUBMITTER: Agarwal S 

PROVIDER: S-EPMC4614821 | biostudies-literature | 2015 Oct

REPOSITORIES: biostudies-literature

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Complex folding and misfolding effects of deer-specific amino acid substitutions in the β2-α2 loop of murine prion protein.

Agarwal Sonya S   Döring Kristina K   Gierusz Leszek A LA   Iyer Pooja P   Lane Fiona M FM   Graham James F JF   Goldmann Wilfred W   Pinheiro Teresa J T TJ   Gill Andrew C AC  

Scientific reports 20151022


The β2-α2 loop of PrP(C) is a key modulator of disease-associated prion protein misfolding. Amino acids that differentiate mouse (Ser169, Asn173) and deer (Asn169, Thr173) PrP(C) appear to confer dramatically different structural properties in this region and it has been suggested that amino acid sequences associated with structural rigidity of the loop also confer susceptibility to prion disease. Using mouse recombinant PrP, we show that mutating residue 173 from Asn to Thr alters protein stabi  ...[more]

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