Host and transmissible spongiform encephalopathy agent strain control glycosylation of PrP

RA Somerville - Journal of general virology, 1999 - microbiologyresearch.org
RA Somerville
Journal of general virology, 1999microbiologyresearch.org
PrP is a host-encoded glycoprotein involved in the pathogenesis of transmissible
spongiform encephalopathies (TSEs) or 'prion'diseases. The normal form of the protein (PrP
(C)) is heavily but incompletely glycosylated; it shows structural diversity in three
neuroanatomically distinct regions of the brain. No effect of TSE infection on PrP (C)
glycosylation has been detected. TSE-specific forms of PrP (PrP (Sc)) vary in their degree of
glycosylation according to strain of TSE infectious agent. PrP (Sc) also varies independently …
PrP is a host-encoded glycoprotein involved in the pathogenesis of transmissible spongiform encephalopathies (TSEs) or ‘prion’ diseases. The normal form of the protein (PrP(C)) is heavily but incompletely glycosylated; it shows structural diversity in three neuroanatomically distinct regions of the brain. No effect of TSE infection on PrP(C) glycosylation has been detected. TSE-specific forms of PrP (PrP(Sc)) vary in their degree of glycosylation according to strain of TSE infectious agent. PrP(Sc) also varies independently in the amount and pattern of glycosylation according to brain region. This diversity shows that the glycosylation of PrP is under both host- and TSE agent-specified control, probably within the biosynthetic pathway for protein N-glycosylation. These findings challenge assumptions that PrP(Sc) is formed from the normal, mature form of PrP(Sc) but are compatible with a model in which the glycosylation phenotype of PrP(Sc) is under the control of both host cellular factors and TSE agent-specified information.
Microbiology Research