Prion transmission between species is governed in part by primary sequence similarity between the infectious prion aggregate, PrP, and the cellular prion protein of the host, PrP A puzzling feature of prion formation is that certain PrP sequences, such as that of bank vole, can be converted by a remarkably broad array of different mammalian prions, whereas others, such as rabbit, show robust resistance to cross-species prion conversion. To examine the structural determinants that confer susceptibility or resistance to prion conversion, we systematically tested over 40 PrP variants of susceptible and resistant PrP sequences in a prion conversion assay. Five key residue positions markedly impacted prion conversion, four of which were in steric zipper segments where side chains from amino acids tightly interdigitate in a dry interface. Strikingly, all five residue substitutions modulating prion conversion involved the gain or loss of an asparagine or glutamine residue. For two of the four positions, Asn and Gln residues were not interchangeable, revealing a strict requirement for either an Asn or Gln residue. Bank voles have a high number of Asn and Gln residues and a high Asn:Gln ratio. These findings suggest that a high number of Asn and Gln residues at specific positions may stabilize β-sheets and lower the energy barrier for cross-species prion transmission, potentially because of hydrogen bond networks from side chain amides forming extended Asn/Gln ladders. These data also suggest that multiple PrP segments containing Asn/Gln residues may act in concert along a replicative interface to promote prion conversion.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5704488PMC
http://dx.doi.org/10.1074/jbc.M117.794107DOI Listing

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