Probing Early Misfolding Events in Prion Protein Mutants by NMR Spectroscopy

The post-translational conversion of the ubiquitously expressed cellular form of the prion protein, PrP(C), into its misfolded and pathogenic isoform, known as prion or PrP(Sc), plays a key role in prion diseases. These maladies are denoted transmissible spongiform encephalopathies (TSEs) and affect both humans and animals. A prerequisite for understanding TSEs is unraveling the molecular mechanism leading to the conversion process whereby most α-helical motifs are replaced by β-sheet secondary structures. Importantly, most point mutations linked to inherited prion diseases are clustered in the C-terminal domain region of PrP(C) and cause spontaneous conversion to PrP(Sc). Structural studies with PrP variants promise new clues regarding the proposed conversion mechanism and may help identify “hot spots” in PrP(C) involved in the pathogenic conversion. These investigations may also shed light on the early structural rearrangements occurring in some PrP(C) epitopes thought to be involved in modulating prion susceptibility. Here we present a detailed overview of our solution-state NMR studies on human prion protein carrying different pathological point mutations and the implications that such findings may have for the future of prion research.