Recombinant scrapie-like prion protein of 106 amino acids is soluble

Abstract

The N terminus of the scrapie isoform of prion protein (PrP^Sc) can be truncated without loss of scrapie infectivity and, correspondingly, the truncation of the N terminus of the cellular isoform, PrP^C, still permits conversion into PrP^Sc. To assess whether additional segments of the PrP molecule can be deleted, we previously removed regions of putative secondary structure in PrP^C; in the present study we found that deletion of each of the four predicted helices prevented PrP^Sc formation, as did deletion of the stop transfer effector region and the C178A mutation. Removal of a 36-residue loop between helices 2 and 3 did not prevent formation of protease-resistant PrP; the resulting scrapie-like protein, designated PrP^Sc106, contained 106 residues after cleavage of an N-terminal signal peptide and a C-terminal sequence for glycolipid anchor addition. Addition of the detergent Sarkosyl to cell lysates solubilized PrP^Sc106, which retained resistance to digestion by proteinase K. These results suggest that all the regions of proposed secondary structure in PrP are required for PrP^Sc formation, as is the disulfide bond stabilizing helices 3 and 4. The discovery of PrP^Sc106 should facilitate structural studies of PrP^Sc, investigations of the mechanism of PrP^Sc formation, and the production of PrP^Sc-specific antibodies.