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. 1999 Mar 19;283(5409):1935-7.
doi: 10.1126/science.283.5409.1935.

Reversible conversion of monomeric human prion protein between native and fibrilogenic conformations

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Reversible conversion of monomeric human prion protein between native and fibrilogenic conformations

G S Jackson et al. Science. .

Abstract

Prion propagation involves the conversion of cellular prion protein (PrPC) into a disease-specific isomer, PrPSc, shifting from a predominantly alpha-helical to beta-sheet structure. Here, conditions were established in which recombinant human PrP could switch between the native alpha conformation, characteristic of PrPC, and a compact, highly soluble, monomeric form rich in beta structure. The soluble beta form (beta-PrP) exhibited partial resistance to proteinase K digestion, characteristic of PrPSc, and was a direct precursor of fibrillar structures closely similar to those isolated from diseased brains. The conversion of PrPC to beta-PrP in suitable cellular compartments, and its subsequent stabilization by intermolecular association, provide a molecular mechanism for prion propagation.

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