Science, Vol.274, No.5295, 2079-2082, 1996
Evidence for the Conformation of the Pathological Isoform of the Prion Protein Enciphering and Propagating Prion Diversity
The fundamental event in prion diseases seems to be a conformational change in cellular prion protein (PrPC) whereby it is converted into the pathologic isoform PrPSc. In fatal familial insomnia (FFI), the protease-resistant fragment of PrPSc after deglycosylation has a size of 19 kilodaltons, whereas that from other inherited and sporadic prion diseases is 21 kilodaltons. Extracts from the brains of FFI patients transmitted disease to transgenic mice expressing a chimeric human-mouse PrP gene about 200 days after inoculation and induced formation of the 19-kilodalton PrPSc fragment, whereas extracts from the brains of familiar and sporadic Creutzfeldt-Jakob disease patients produced the 21-kilodalton PrPSc fragment in these mice. The results presented indicate that the conformation of PrPSc functions as a template in directing the formation of nascent PrPSc and suggest a mechanism to explain strains of prions where diversity is encrypted in the conformation of PrPSc.
Keywords:FATAL FAMILIAL INSOMNIA;CREUTZFELDT-JAKOB-DISEASE;TRANSMISSIBLE MINK ENCEPHALOPATHY;GERSTMANN-STRAUSSLER SYNDROME;DNA POLYMORPHISM;TRANSGENIC MICE;AGENT-STRAIN;SCRAPIE;MOUSE;GENE