Prion gene paralogs are dispensable for early zebrafish development and have nonadditive roles in seizure susceptibility

Patricia L A Leighton; Richard Kanyo; Gavin J Neil; Niall M Pollock; W Ted Allison

doi:10.1074/jbc.RA117.001171

Prion gene paralogs are dispensable for early zebrafish development and have nonadditive roles in seizure susceptibility

J Biol Chem. 2018 Aug 10;293(32):12576-12592. doi: 10.1074/jbc.RA117.001171. Epub 2018 Jun 14.

Authors

Patricia L A Leighton¹, Richard Kanyo¹, Gavin J Neil¹, Niall M Pollock¹, W Ted Allison²

Affiliations

¹ From the Department of Biological Sciences and the Centre for Prion and Protein Folding Diseases, University of Alberta, Edmonton, Alberta T6G 2E9, Canada.
² From the Department of Biological Sciences and the Centre for Prion and Protein Folding Diseases, University of Alberta, Edmonton, Alberta T6G 2E9, Canada ted.allison@ualberta.ca.

Abstract

Normally folded prion protein (PrP^C) and its functions in healthy brains remain underappreciated compared with the intense study of its misfolded forms ("prions," PrP^Sc) during the pathobiology of prion diseases. This impedes the development of therapeutic strategies in Alzheimer's and prion diseases. Disrupting the zebrafish homologs of PrP^C has provided novel insights; however, mutagenesis of the zebrafish paralog prp2 did not recapitulate previous dramatic developmental phenotypes, suggesting redundancy with the prp1 paralog. Here, we generated zebrafish prp1 loss-of-function mutant alleles and dual prp1^-/-;prp2^-/- mutants. Zebrafish prp1^-/- and dual prp1^-/-;prp2^-/- mutants resemble mammalian Prnp knockouts insofar as they lack overt phenotypes, which surprisingly contrasts with reports of severe developmental phenotypes when either prp1 or prp2 is knocked down acutely. Previous studies suggest that PrP^C participates in neural cell development/adhesion, including in zebrafish where loss of prp2 affects adhesion and deposition patterns of lateral line neuromasts. In contrast with the expectation that prp1's functions would be redundant to prp2, they appear to have opposing functions in lateral line neurodevelopment. Similarly, loss of prp1 blunted the seizure susceptibility phenotypes observed in prp2 mutants, contrasting the expected exacerbation of phenotypes if these prion gene paralogs were serving redundant roles. In summary, prion mutant fish lack the overt phenotypes previously predicted, and instead they have subtle phenotypes similar to mammals. No evidence was found for functional redundancy in the zebrafish prion gene paralogs, and the phenotypes observed when each gene is disrupted individually are consistent with ancient functions of prion proteins in neurodevelopment and modulation of neural activity.

Keywords: PrPC; TALEN; excitotoxicity; gene editing; neural hyperactivity; neurodegeneration; neurodevelopment; prion disease; targeted mutagenesis; transcription activator-like effector nuclease; zebrafish.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Animals, Genetically Modified / genetics
Animals, Genetically Modified / growth & development*
Gene Expression Regulation, Developmental*
Mutation
Neurogenesis / genetics*
Phenotype
Prion Diseases / physiopathology*
Prion Proteins / genetics*
Seizures / physiopathology*
Zebrafish / genetics
Zebrafish / growth & development*

Substances

Prion Proteins