BSE prions propagate as either variant CJD-like or sporadic CJD-like prion strains in transgenic mice expressing human prion protein

Asante, Emmanuel A.; Linehan, Jacqueline M.; Desbruslais, Melanie; Joiner, Susan; Gowland, Ian; Wood, Andrew L.; Welch, Julie L.; Hill, Andrew F.; Lloyd, Sarah E.; Wadsworth, Jonathan D. F.; Collinge, John

doi:10.1093/emboj/cdf653

Cited by 325 publications

(382 citation statements)

References 33 publications

Supporting

Mentioning

354

Contrasting

Unclassified

Order By: Relevance

“…Experimental confirmation that variant CreutzfeldtJakob disease (vCJD) [1] is caused by the same prion strain as that causing bovine spongiform encephalopathy (BSE) in cattle [2][3][4][5] led to global concern that human exposure to BSE prions posed a significant threat to public health [6][7][8]. While the risk of new dietary exposure to BSE prions in the UK is now remote [9], the majority of the UK population may have been exposed during the late 1980s and early 1990s.…”

Section: Introductionmentioning

confidence: 99%

“…Owing to the paucity of tissue available, it was not possible to inoculate different lines of transgenic mice expressing either human PrP 129 methionine or valine. Based on our experience of the transmission properties of vCJD and BSE prions, we chose to use Tg45 mice homozygous for 129 methionine [5]. These mice faithfully propagate the molecular and neuropathological phenotype of vCJD following primary challenge with either vCJD prions [5,57] or BSE prions [5] and are known to be sensitive to infection when inoculated with vCJD peripheral tissue containing PrP Sc at a concentration 10 4.7 -fold lower than in brain [57].…”

Section: Introductionmentioning

confidence: 99%

“…Based on our experience of the transmission properties of vCJD and BSE prions, we chose to use Tg45 mice homozygous for 129 methionine [5]. These mice faithfully propagate the molecular and neuropathological phenotype of vCJD following primary challenge with either vCJD prions [5,57] or BSE prions [5] and are known to be sensitive to infection when inoculated with vCJD peripheral tissue containing PrP Sc at a concentration 10 4.7 -fold lower than in brain [57]. Importantly, the novel prion strain (associated with type 5 PrP Sc ) that is generated in vCJD-challenged human PrP 129V transgenic mice also transmits infection efficiently to transgenic mice expressing human PrP 129M [51].…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Effect of fixation on brain and lymphoreticular vCJD prions and bioassay of key positive specimens from a retrospective vCJD prevalence study

Wadsworth

Dalmau-Mena

Joiner

et al. 2010

The Journal of Pathology

View full text Add to dashboard Cite

Anonymous screening of lymphoreticular tissues removed during routine surgery has been applied to estimate the UK population prevalence of asymptomatic vCJD prion infection. The retrospective study of Hilton et al (J Pathol 2004; 203: 733-739) found accumulation of abnormal prion protein in three formalin-fixed appendix specimens. This led to an estimated UK prevalence of vCJD infection of ∼1 in 4000, which remains the key evidence supporting current risk reduction measures to reduce iatrogenic transmission of vCJD prions in the UK. Confirmatory testing of these positives has been hampered by the inability to perform immunoblotting of formalin-fixed tissue. Animal transmission studies offer the potential for 'gold standard' confirmatory testing but are limited by both transmission barrier effects and known effects of fixation on scrapie prion titre in experimental models. Here we report the effects of fixation on brain and lymphoreticular human vCJD prions and comparative bioassay of two of the three prevalence study formalin-fixed, paraffin-embedded (FFPE) appendix specimens using transgenic mice expressing human prion protein (PrP). While transgenic mice expressing human PrP 129M readily reported vCJD prion infection after inoculation with frozen vCJD brain or appendix, and also FFPE vCJD brain, no infectivity was detected in FFPE vCJD spleen. No prion transmission was observed from either of the FFPE appendix specimens. The absence of detectable infectivity in fixed, known positive vCJD lymphoreticular tissue precludes interpreting negative transmissions from vCJD prevalence study appendix specimens. In this context, the Hilton et al study should continue to inform risk assessment pending the outcome of larger-scale studies on discarded surgical tissues and autopsy samples.

show abstract

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Effect of fixation on brain and lymphoreticular vCJD prions and bioassay of key positive specimens from a retrospective vCJD prevalence study

Wadsworth

Dalmau-Mena

Joiner

et al. 2010

The Journal of Pathology

View full text Add to dashboard Cite

show abstract

“…-mapping PrP regions involved in or required for PrP conversion and prion replication [36,37,44,56,57,63,78,80]; -studies on the physiological role of PrP C and the contributions of individual molecular regions to these functions [65]; -studies on molecular aspects of species barrier effects by mutation of single or limited numbers of positions within the PrP [20,41,51,76,77,82]; -modelling of familial forms of human prion diseases [3,4,60]; -analysis of the cell specificity of prion propagation [48,71,72]; -analysis of the role of PrP glycosylation [22,64]; -studies on the mechanisms of prion spread [11,12]; -studies on the neuropathological roles of PrP C and of PrP D in prion disease [39]; -studies on the function of PrP Doppel [34].…”

Section: Mutant Prp Expression Modelsmentioning

confidence: 99%

“…represented only one defined strain when reisolated from a variety of species (including vCJD in humans) which were infected during the course of the BSE epidemic in the UK. Asante et al [3] have reported that the transmission of BSE to Tg35 mice overexpressing human PrP C produced primarily the well known vCJD PrP D phenotype, but also in low numbers a second phenotype (distinguished by biochemical and anatomical analysis of the PrP D deposits) which was reminiscent of sporadic CJD PrP D . Another publication describes the transmission of a new bovine prion strain called bovine amyloidotic spongiform encephalopathy (BASE), which can be discriminated from BSE mainly on the basis of a lower molecular mass of the unglycosylated form of PrP D , a different anatomical distribution of the accumulated PrP D in the brain, and by the presence of PrP immunoreactive amyloid plaques, bovine PrP transgenic mice.…”

Section: Phenotypic And/or Biological Evolution Of Prion Strains As Amentioning

confidence: 99%

Rodent models for prion diseases

Groschup

Buschmann

2008

Vet. Res.

View full text Add to dashboard Cite

-Until today most prion strains can only be propagated and the infectivity content assayed by experimentally challenging conventional or transgenic animals. Robust cell culture systems are not available for any of the natural and only for a few of the experimental prion strains. Moreover, the pathogenesis of different transmissible spongiform encephalopathies (TSE) can be analysed systematically by using experimentally infected animals. While, in the beginning, animals belonging to the natural host species were used, more and more rodent model species have been established, mostly due to practical reasons. Nowadays, most of these experiments are performed using highly susceptible transgenic mouse lines expressing cellular prion proteins, PrP, from a variety of species like cattle, sheep, goat, cervidae, elk, hamster, mouse, mink, pig, and man. In addition, transgenic mice carrying specific mutations or polymorphisms have helped to understand the molecular pathomechanisms of prion diseases. Transgenic mouse models have been utilised to investigate the physiological role of PrP C , molecular aspects of species barrier effects, the cell specificity of the prion propagation, the role of the PrP glycosylation, the mechanisms of the prion spread, the neuropathological roles of PrP C and of its abnormal isoform PrP D (D for disease) as well as the function of PrP Doppel. Transgenic mouse models have also been used for mapping of PrP regions involved in or required for the PrP conversion and prion replication as well as for modelling of familial forms of human prion diseases.

show abstract

Prions

Prusiner

2006

Encyclopedia of Molecular Cell Biology and Molecular Medicine

View full text Add to dashboard Cite

BSE prions propagate as either variant CJD-like or sporadic CJD-like prion strains in transgenic mice expressing human prion protein

Cited by 325 publications

References 33 publications

Effect of fixation on brain and lymphoreticular vCJD prions and bioassay of key positive specimens from a retrospective vCJD prevalence study

Effect of fixation on brain and lymphoreticular vCJD prions and bioassay of key positive specimens from a retrospective vCJD prevalence study

Rodent models for prion diseases

Prions

Contact Info

Product

Resources

About