RÉSUMÉ
Transgenic mice expressing human prion protein in the absence of endogenous mouse prion protein faithfully replicate human prions. These models reproduce all of the key features of human disease, including long clinically silent incubation periods prior to fatal neurodegeneration with neuropathological phenotypes that mirror human prion strain diversity. Critical contributions to our understanding of human prion disease pathogenesis and aetiology have only been possible through the use of transgenic mice. These models have provided the basis for the conformational selection model of prion transmission barriers and have causally linked bovine spongiform encephalopathy with variant Creutzfeldt-Jakob disease. In the future these models will be essential for evaluating newly identified potentially zoonotic prion strains, for validating effective methods of prion decontamination and for developing effective therapeutic treatments for human prion disease.
Sujet(s)
Animal génétiquement modifié/physiologie , Maladies à prions/génétique , Maladies à prions/anatomopathologie , Animaux , Bovins , Modèles animaux de maladie humaine , Humains , Souris , Souris transgéniques , Phénotype , Prions/classification , Prions/génétique , Prions/physiologieSujet(s)
Maladies chez les jumeaux/épidémiologie , Maladies à prions/épidémiologie , Jumeaux monozygotes , Âge de début , Encéphale/métabolisme , Encéphale/anatomopathologie , Maladie de Creutzfeldt-Jakob/métabolisme , Maladies chez les jumeaux/génétique , Maladies chez les jumeaux/anatomopathologie , Environnement , Femelle , Humains , Adulte d'âge moyen , Pedigree , Protéines PrPSc/métabolisme , Maladies à prions/génétique , Maladies à prions/anatomopathologie , Protéines prion , Prions/génétique , Analyse de séquence d'ADNRÉSUMÉ
BACKGROUND: Human prion diseases have sporadic, acquired and inherited etiologies and show considerable phenotypic heterogeneity. An individual inherited prion disease offers an opportunity to study the determinants of this clinicopathologic heterogeneity among individuals with the same causal mutation. METHODS: We report clinical and pathologic data from three families with different 5-octapeptide repeat insertion (5-OPRI) mutations of the prion protein gene (PRNP), extending the reported phenotypic range of this mutation. RESULTS: The proband of a South African family presented with a rapidly progressive dementia and atypical pathology associated with kuru-like prion protein plaques. The original mutation in this family probably occurred on a PRNP allele encoding a 1-octapeptide repeat deletion polymorphism. This has not been previously reported as a precursor allele in over 30 other OPRI mutation kindreds. An English family with a genetically distinct mutation but identical protein product showed clinical onsets that varied 30 years between father and daughter, an effect that may be explained by their genotypes at PRNP codon 129. A patient from Northern Ireland with a phenotype of sporadic Creutzfeldt-Jakob disease presenting with visual disturbance was unexpectedly found to have a 5-OPRI. CONCLUSIONS: When these cases were combined with the existing world literature, the mean age at onset for patients with 5-octapeptide repeat insertion (5-OPRI) was significantly later than that for patients with 6-OPRI, but both mutations exhibit a similar powerful disease modifying effect of PRNP codon 129.
Sujet(s)
Prédisposition génétique à une maladie/génétique , Mutation/génétique , Maladies à prions/génétique , Prions/génétique , Séquences répétées d'acides aminés/génétique , Adulte , Codon/génétique , Analyse de mutations d'ADN , Évolution de la maladie , Femelle , Dépistage génétique , Génotype , Humains , Mâle , Adulte d'âge moyen , Irlande du Nord , Pedigree , Phénotype , Polymorphisme génétique/génétique , Maladies à prions/ethnologie , Maladies à prions/métabolisme , République d'Afrique du SudRÉSUMÉ
BACKGROUND: Disease-related prion protein (PrP(Sc)) is readily detectable in lymphoreticular tissues in variant Creutzfeldt-Jakob disease (vCJD), but not in other forms of human prion disease. This distinctive pathogenesis, with the unknown population prevalence of asymptomatic vCJD infection, has led to significant concerns that secondary transmission of vCJD prions will occur through a wide range of surgical procedures. To date PrP(Sc):prion infectivity ratios have not been determined in vCJD, and it is unknown whether vCJD prions are similar to experimental rodent prions, where PrP(Sc) concentration typically reflects infectious prion titre. AIM: To investigate prion infectivity in vCJD tissue containing barely detectable levels of PrP(Sc). METHODS: Transgenic mice expressing only human PrP (Tg(HuPrP129M(+/+)Prnp(o/o))-35 and Tg(HuPrP129M(+/+)Prnp(o/o))-45 mice) were inoculated with brain or rectal tissue from a previously characterised patient with vCJD. These tissues contain the maximum and minimum levels of detectable PrP(Sc) that have been observed in vCJD. RESULTS: Efficient transmission of prion infection was observed in transgenic mice inoculated with vCJD rectal tissue containing PrP(Sc) at a concentration of 10(4.7)-fold lower than that in vCJD brain. CONCLUSIONS: These data confirm the potential risks for secondary transmission of vCJD prions via gastrointestinal procedures and support the use of PrP(Sc) as a quantitative marker of prion infectivity in vCJD tissues.
