Convergent generation of atypical prions in knockin mouse models of genetic prion disease
Surabhi Mehra, … , Walker S. Jackson, Joel C. Watts
Surabhi Mehra, … , Walker S. Jackson, Joel C. Watts
Published August 1, 2024
Citation Information: J Clin Invest. 2024;134(15):e176344. https://doi.org/10.1172/JCI176344.
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Research Article Neuroscience

Convergent generation of atypical prions in knockin mouse models of genetic prion disease

Abstract

Most cases of human prion disease arise due to spontaneous misfolding of WT or mutant prion protein, yet recapitulating this event in animal models has proven challenging. It remains unclear whether spontaneous prion generation can occur within the mouse lifespan in the absence of protein overexpression and how disease-causing mutations affect prion strain properties. To address these issues, we generated knockin mice that express the misfolding-prone bank vole prion protein (BVPrP). While mice expressing WT BVPrP (I109 variant) remained free from neurological disease, a subset of mice expressing BVPrP with mutations (D178N or E200K) causing genetic prion disease developed progressive neurological illness. Brains from spontaneously ill knockin mice contained prion disease–specific neuropathological changes as well as atypical protease-resistant BVPrP. Moreover, brain extracts from spontaneously ill D178N- or E200K-mutant BVPrP–knockin mice exhibited prion seeding activity and transmitted disease to mice expressing WT BVPrP. Surprisingly, the properties of the D178N- and E200K-mutant prions appeared identical before and after transmission, suggesting that both mutations guide the formation of a similar atypical prion strain. These findings imply that knockin mice expressing mutant BVPrP spontaneously develop a bona fide prion disease and that mutations causing prion diseases may share a uniform initial mechanism of action.

Authors

Surabhi Mehra, Matthew E.C. Bourkas, Lech Kaczmarczyk, Erica Stuart, Hamza Arshad, Jennifer K. Griffin, Kathy L. Frost, Daniel J. Walsh, Surachai Supattapone, Stephanie A. Booth, Walker S. Jackson, Joel C. Watts

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Figure 2

Knockin mice expressing mutant bank vole PrP develop spontaneous neurological illness.

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Knockin mice expressing mutant bank vole PrP develop spontaneous neurolo...
(A) Kaplan-Meier curves for the development of signs of neurological illness in kiBVIWT (black, n = 22), kiBVIE200K (red, n = 23), and kiBVID178N (blue, n = 23) mice. Statistical significance was assessed using the log-rank test. (B) Analysis of sex-specific effects on the age of onset of spontaneous neurological illness (mean ± SD) in kiBVIE200K (left graph; n = 11 for males, n = 3 for females) and kiBVID178N (right graph; n = 8 for males, n = 7 for females) mice. Statistical significance was assessed using unpaired, 2-tailed Mann-Whitney tests. (C) Heatmaps for commonly observed signs of neurological illness in kiBVIE200K (left, n = 14) and kiBVID178N (right, n = 15) mice that developed spontaneous disease at the indicated ages. Each row represents a single mouse, and symptoms were designated as absent (white; score = 0), moderate (light blue; score = 1), or severe (dark blue; score = 2).