Prion (Dec 2023)

Insight into the conserved structural dynamics of the C-terminus of mammal PrPC identifies structural core and possible structural role of pharmacological chaperones

  • Patricia Soto,
  • Garrett M. Gloeb,
  • Kaitlin A. Tsuchida,
  • Austin A. Charles,
  • Noah M. Greenwood,
  • Heidi Hendrickson

DOI
https://doi.org/10.1080/19336896.2023.2186674
Journal volume & issue
Vol. 17, no. 1
pp. 55 – 66

Abstract

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ABSTRACTMisfolding of the prion protein is central to prion disease aetiology. Although understanding the dynamics of the native fold helps to decipher the conformational conversion mechanism, a complete depiction of distal but coupled prion protein sites common across species is lacking. To fill this gap, we used normal mode analysis and network analysis to examine a collection of prion protein structures deposited on the protein data bank. Our study identified a core of conserved residues that sustains the connectivity across the C-terminus of the prion protein. We propose how a well-characterized pharmacological chaperone may stabilize the fold. Also, we provide insight into the effect on the native fold of initial misfolding pathways identified by others using kinetics studies.

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