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Prions Genetic Polymorphism & Susceptibility. Carlos Francisco Mendoza. Human Prion Diseases. Comparison of Prp C and Prp Sc. Evidence Supports the Prion Hypothesis. Genetic Polymorphism. RPSA Polymorphisms have no direct influence on susceptibility to sporadic CJD. Susceptibility.
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PrionsGenetic Polymorphism & Susceptibility Carlos Francisco Mendoza
Genetic Polymorphism RPSA Polymorphisms have no direct influence on susceptibility to sporadic CJD
Susceptibility Post-mortem Immunocytochemistry Showing partial Protease Resistance
Disease Transmission and Species Barrier Anne Busch
Introduction • Infectious protein agent w/o DNA or RNA • Progressive neurodegenerative diseases: Scrapie, CJD, BSE • In humans : dementia • In other animals : ataxia • Genetic, infectious, sporadic in origin • Involve modified isoform of PrP (mammals) • PrPsc: misfolded • PrPc: normal, constitutively expressed in healthy brain
Normal protein → infectious, pathogenic protease resistant protein • Exogenous PrPsc or overproduction of PrpC can cause disease • Brain extracts without pathogenic isoform can be infectious (mice models infected with bovine PrpSC are infectious but PrPSC undetectable) → maybe its not only a protein? • Prpc → prp* & host specific prpsc • Dynamic bistability & threshold properties
Conversion of PrPc to PrPsc • α- helix and coil structure -> β-sheet • PrPsc: 30% alphahelix, 45% beta sheet while PrpC is 30% alpha and a little beta (from FITR and CD studies) • PrPsc • 1* structure determined by Prp gene of host • Misfoldedisoform acts as template to convert PrPc into PrPsc within the cell • Faciliated by another protein • Resistant to proteolytic cleavage -> accumulation of extracellular plaques • Only differ in conformation? • One primary structure can lead to multiple conformations?
Infectious conversion not yet demonstrated in vivo BUT have shown PrP conversion to a protease resistant isoform, like PrPsc
Interspecies transmission Tissue from diseased cattle can infect mice, sheep, pigs, mink after intracerebralinjection Prolonged incubation period upon first passage into new host= species barrier De novo prions reflect host PrP sequence, not PrPsc sequence from donor Incubation time shortens upon subsequent passage into the new host
Species barrier • Due to differences in PrP sequence between species • Serial passage (intraspecies): incubation period shortens & pathological properties stabilize • After 3 passages incubation period stable → suggests intermediate conformation in primary infection PrP* which catalyzes formation of host PrPSC, which is autocatalytic
Species barrier • Depends on kinetic characteristics of of the conversion reaction of the prion protein
Factors contributing to Species Barrier • Difference in Prp sequence from donor to host • Depends on host • Species specificity of protein X: factor binds PrpC and facilitates conversion • Little is known about factor X but it assumed to be a protein
3. Strain of prion • encoded in conformation and together with sequence determines tertiary structure • Infectious material from different sources produces distinct and reproducible patterns of incubation time, proteolytic resistance/cleavage, and distribution within the CNS
How can a genetic disease become infectious? • Conformational templating • Mechanism for generation and propagation • System with dynamic bistability and threshold properties
References Diego Kaski, Prion Diseases, Medicine 37:11, 2009 Wen-QuanZou, Modeling of human prions and prion diseases in vitro and in vivo, Vol. I, No. 2, 2004 Masato Enari, Scrapie prion protein accumulation by scrapie-infected neuroblastomacells abrogated by exposure to a prion protein antibody, PNAS, 9295-9299, 2001 Rodrigo Morales, The prion strain phenomenon: Molecular basis and unprecedented features, BBA, 681-691, 2007 Jisuk Yun, The first report of RPSA polymorphisms, also called 37/67kDa LRP/LR gene, in sporadic Creutzfeldt-Jakob disease (CJD).
