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Peer-reviewed veterinary case report

Regulated coexpression of PrP from different species in mice impacts the replication and host range properties of prion strains.

Journal:
Proceedings of the National Academy of Sciences of the United States of America
Year:
2025
Authors:
DeFranco, Joseph P et al.
Affiliation:
Department of Microbiology · United States
Species:
rodent

Abstract

Our previous demonstration that replacement of murine cellular prion protein (PrP) expression with elk or deer PrPeliminated the resistance of mice to chronic wasting disease (CWD) prions from deer, elk, and other cervids highlighted the importance of sequence homology between PrPand its conformationally altered counterpart (PrP) for optimal prion replication. To further investigate the effects of species-specific PrP primary structural variation on the evolution of prion host range and strain properties during interspecies transmissions, we generated mice with precisely controlled expression of both murine and either deer or elk PrPand challenged them with cervid or murine prions. While CWD prion transmission was inhibited to varying degrees under these conditions, the strain properties and species specificities of the resulting cervid prions were not impacted. By contrast, although murine prions induced conformational conversion of mouse but not coexpressed cervid PrP, the resulting prions produced disease in mice expressing either cervid or mouse PrP. Our findings show that while mouse PrPinhibited conformational conversion of deer or elk PrPwithout affecting the host range of CWD prions, coexpression of cervid PrPinfluenced the selection of strains with expanded host range properties during conformational conversion of mouse PrPby murine prions. Our studies reveal diverse influences of bystander PrPexpression on the replication, host range, and strain properties of prions generated during conformational conversion of their coexpressed cognate PrP. These cooperative or inhibitory effects occurand derive from species-specific primary structural variations between coexpressed PrPsubstrates and infectious prions.

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Original publication: https://pubmed.ncbi.nlm.nih.gov/41296716/