PLoS ONE (Feb 2010)

Unexpected tolerance of alpha-cleavage of the prion protein to sequence variations.

  • José B Oliveira-Martins,
  • Sei-ichi Yusa,
  • Anna Maria Calella,
  • Claire Bridel,
  • Frank Baumann,
  • Paolo Dametto,
  • Adriano Aguzzi

DOI
https://doi.org/10.1371/journal.pone.0009107
Journal volume & issue
Vol. 5, no. 2
p. e9107

Abstract

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The cellular form of the prion protein, PrP(C), undergoes extensive proteolysis at the alpha site (109K [see text]H110). Expression of non-cleavable PrP(C) mutants in transgenic mice correlates with neurotoxicity, suggesting that alpha-cleavage is important for PrP(C) physiology. To gain insights into the mechanisms of alpha-cleavage, we generated a library of PrP(C) mutants with mutations in the region neighbouring the alpha-cleavage site. The prevalence of C1, the carboxy adduct of alpha-cleavage, was determined for each mutant. In cell lines of disparate origin, C1 prevalence was unaffected by variations in charge and hydrophobicity of the region neighbouring the alpha-cleavage site, and by substitutions of the residues in the palindrome that flanks this site. Instead, alpha-cleavage was size-dependently impaired by deletions within the domain 106-119. Almost no cleavage was observed upon full deletion of this domain. These results suggest that alpha-cleavage is executed by an alpha-PrPase whose activity, despite surprisingly limited sequence specificity, is dependent on the size of the central region of PrP(C).