Crossing the Species Barrier by PrPSc Replication In Vitro Generates Unique Infectious Prions

Castilla, Joaquı́n; Gonzalez-Romero, Dennisse; Saá, Paula; Morales, Rodrigo; Castro, Jorge de; Soto, Claudio

doi:10.1016/j.cell.2008.07.030

Cited by 187 publications

(187 citation statements)

References 48 publications

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“…However, under other conditions where higher amounts of input seed and increased cycles per round were used, PMCA conversion even across a resistant species barrier has been reported (28). In our experiments using conditions similar to those previously described (21), no significant differences in clinical signs, incubation periods, and histopathological or biochemical data were found between animals inoculated with brain-derived input seed or PMCA-derived products from rounds 4, 6, and 8.…”

Section: Discussionmentioning

confidence: 43%

“…As opposed to earlier studies where prion infectivity was often assayed in material from a single round after >15 serial rounds of PMCA (21-24), we analyzed multiple early rounds of several different hamster and transgenic mouse PMCA experiments. Furthermore, to estimate infectivity titers all but one (22) of these earlier studies used an incubation time assay based on a standard curve using brain-derived prion infectivity (25), but such a standard curve may not be valid for PMCA-derived infectivity (26,27), especially if a new prion strain is generated (28). In contrast, in the present experiments the use of end-point dilution titrations enabled us to follow the disappearance of the input infectivity in control reactions and accurately titer any newly generated infectivity.…”

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confidence: 99%

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Lower specific infectivity of protease-resistant prion protein generated in cell-free reactions

Klingeborn

Race

Meade-White

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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Prions are unconventional infectious agents that cause transmissible spongiform encephalopathy (TSE) diseases, or prion diseases. The biochemical nature of the prion infectious agent remains unclear. Previously, using a protein misfolding cyclic amplification (PMCA) reaction, infectivity and disease-associated protease-resistant prion protein (PrPres) were both generated under cell-free conditions, which supported a nonviral hypothesis for the agent. However, these studies lacked comparative quantitation of both infectivity titers and PrPres, which is important both for biological comparison with in vivo-derived infectivity and for excluding contamination to explain the results. Here during four to eight rounds of PMCA, end-point dilution titrations detected a >320-fold increase in infectivity versus that in controls. These results provide strong support for the hypothesis that the agent of prion infectivity is not a virus. PMCA-generated samples caused the same clinical disease and neuropathology with the same rapid incubation period as the input brain-derived scrapie samples, providing no evidence for generation of a new strain in PMCA. However, the ratio of the infectivity titer to the amount of PrPres (specific infectivity) was much lower in PMCA versus brain-derived samples, suggesting the possibility that a substantial portion of PrPres generated in PMCA might be noninfectious.Creutzfeldt-Jakob disease | amyloid | neurodegeneration | protein polymerization | protein aggregation

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Section: Discussionmentioning

confidence: 43%

mentioning

confidence: 99%

Lower specific infectivity of protease-resistant prion protein generated in cell-free reactions

Klingeborn

Race

Meade-White

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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“…In serial PMCA, prions replicate indefinitely through successive rounds of dilutions and amplification, and this strategy has been used to traverse species barriers and generate species-adapted prions (35). Because sPMCA generated infectious rabbit prions, a species that was considered resistant to prion disease (36), we used the same approach to produce horse prions.…”

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confidence: 99%

Prion replication without host adaptation during interspecies transmissions

Bian

Khaychuk

Angers

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Adaptation of prions to new species is thought to reflect the capacity of the host-encoded cellular form of the prion protein (PrPC) to selectively propagate optimized prion conformations from larger ensembles generated in the species of origin. Here we describe an alternate replicative process, termed nonadaptive prion amplification (NAPA), in which dominant conformers bypass this requirement during particular interspecies transmissions. To model susceptibility of horses to prions, we produced transgenic (Tg) mice expressing cognate PrPC. Although disease transmission to only a subset of infected TgEq indicated a significant barrier to EqPrPCconversion, the resulting horse prions unexpectedly failed to cause disease upon further passage to TgEq. TgD expressing deer PrPCwas similarly refractory to deer prions from diseased TgD infected with mink prions. In both cases, the resulting prions transmitted to mice expressing PrPCfrom the species of prion origin, demonstrating that transmission barrier eradication of the originating prions was ephemeral and adaptation superficial in TgEq and TgD. Horse prions produced in vitro by protein misfolding cyclic amplification of mouse prions using horse PrPCalso failed to infect TgEq but retained tropism for wild-type mice. Concordant patterns of neuropathology and prion deposition in susceptible mice infected with NAPA prions and the corresponding prion of origin confirmed preservation of strain properties. The comparable responses of both prion types to guanidine hydrochloride denaturation indicated this occurs because NAPA precludes selection of novel prion conformations. Our findings provide insights into mechanisms regulating interspecies prion transmission and a framework to reconcile puzzling epidemiological features of certain prion disorders.

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“…The prion protein has two distinct isoforms, the non-infectious host-encoded protein (PrP . This technique has proven to effectively recapitulate the species and strain specificity of PrP Sc conversion from PrP C , to emulate prion strain interference, and to amplify very low levels of PrP Sc from infected tissues, fluids, and environmental samples 6,7,16,23 . This paper details the PMCA protocol, including recommendations for minimizing contamination, generating consistent results, and quantifying those results.…”

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confidence: 99%

Protein Misfolding Cyclic Amplification of Prions

Saunders

Bartz

Shikiya

2012

JoVE

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Prions are infectious agents that cause the inevitably fatal transmissible spongiform encephalopathy (TSE) in animals and humans 9,18 . The prion protein has two distinct isoforms, the non-infectious host-encoded protein (PrP . This technique has proven to effectively recapitulate the species and strain specificity of PrP Sc conversion from PrP C , to emulate prion strain interference, and to amplify very low levels of PrP Sc from infected tissues, fluids, and environmental samples 6,7,16,23 . This paper details the PMCA protocol, including recommendations for minimizing contamination, generating consistent results, and quantifying those results. We also discuss several PMCA applications, including generation and characterization of infectious prion strains, prion strain interference, and the detection of prions in the environment. Video LinkThe video component of this article can be found at

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Crossing the Species Barrier by PrPSc Replication In Vitro Generates Unique Infectious Prions

Cited by 187 publications

References 48 publications

Lower specific infectivity of protease-resistant prion protein generated in cell-free reactions

Lower specific infectivity of protease-resistant prion protein generated in cell-free reactions

Prion replication without host adaptation during interspecies transmissions

Protein Misfolding Cyclic Amplification of Prions

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