New and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the Prnp gene

Chronic wasting disease (CWD) is a prion disease affecting cervids. Polymorphisms in the prion protein gene can result in extended survival of CWD-infected animals. However, the impact of polymorphisms on cellular prion protein (PrP(C)) and prion properties is less understood. Previously, we charact...

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Autores principales: Hannaoui, Samia, Triscott, Elizabeth, Duque Velásquez, Camilo, Chang, Sheng Chun, Arifin, Maria Immaculata, Zemlyankina, Irina, Tang, Xinli, Bollinger, Trent, Wille, Holger, McKenzie, Debbie, Gilch, Sabine
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8341689/
https://www.ncbi.nlm.nih.gov/pubmed/34310662
http://dx.doi.org/10.1371/journal.ppat.1009795
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author Hannaoui, Samia
Triscott, Elizabeth
Duque Velásquez, Camilo
Chang, Sheng Chun
Arifin, Maria Immaculata
Zemlyankina, Irina
Tang, Xinli
Bollinger, Trent
Wille, Holger
McKenzie, Debbie
Gilch, Sabine
author_facet Hannaoui, Samia
Triscott, Elizabeth
Duque Velásquez, Camilo
Chang, Sheng Chun
Arifin, Maria Immaculata
Zemlyankina, Irina
Tang, Xinli
Bollinger, Trent
Wille, Holger
McKenzie, Debbie
Gilch, Sabine
author_sort Hannaoui, Samia
collection PubMed
description Chronic wasting disease (CWD) is a prion disease affecting cervids. Polymorphisms in the prion protein gene can result in extended survival of CWD-infected animals. However, the impact of polymorphisms on cellular prion protein (PrP(C)) and prion properties is less understood. Previously, we characterized the effects of a polymorphism at codon 116 (A>G) of the white-tailed deer (WTD) prion protein and determined that it destabilizes PrP(C) structure. Comparing CWD isolates from WTD expressing homozygous wild-type (116AA) or heterozygous (116AG) PrP, we found that 116AG-prions were conformationally less stable, more sensitive to proteases, with lower seeding activity in cell-free conversion and reduced infectivity. Here, we aimed to understand CWD strain emergence and adaptation. We show that the WTD-116AG isolate contains two different prion strains, distinguished by their host range, biochemical properties, and pathogenesis from WTD-116AA prions (Wisc-1). Serial passages of WTD-116AG prions in tg(CerPrP)1536(+/+) mice overexpressing wild-type deer-PrP(C) revealed two populations of mice with short and long incubation periods, respectively, and remarkably prolonged clinical phase upon inoculation with WTD-116AG prions. Inoculation of serially diluted brain homogenates confirmed the presence of two strains in the 116AG isolate with distinct pathology in the brain. Interestingly, deglycosylation revealed proteinase K-resistant fragments with different electrophoretic mobility in both tg(CerPrP)1536(+/+) mice and Syrian golden hamsters infected with WTD-116AG. Infection of tg60 mice expressing deer S96-PrP with 116AG, but not Wisc-1 prions induced clinical disease. On the contrary, bank voles resisted 116AG prions, but not Wisc-1 infection. Our data indicate that two strains co-existed in the WTD-116AG isolate, expanding the variety of CWD prion strains. We argue that the 116AG isolate does not contain Wisc-1 prions, indicating that the presence of 116G-PrP(C) diverted 116A-PrP(C) from adopting a Wisc-1 structure. This can have important implications for their possible distinct capacities to cross species barriers into both cervids and non-cervids.
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spelling pubmed-83416892021-08-06 New and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the Prnp gene Hannaoui, Samia Triscott, Elizabeth Duque Velásquez, Camilo Chang, Sheng Chun Arifin, Maria Immaculata Zemlyankina, Irina Tang, Xinli Bollinger, Trent Wille, Holger McKenzie, Debbie Gilch, Sabine PLoS Pathog Research Article Chronic wasting disease (CWD) is a prion disease affecting cervids. Polymorphisms in the prion protein gene can result in extended survival of CWD-infected animals. However, the impact of polymorphisms on cellular prion protein (PrP(C)) and prion properties is less understood. Previously, we characterized the effects of a polymorphism at codon 116 (A>G) of the white-tailed deer (WTD) prion protein and determined that it destabilizes PrP(C) structure. Comparing CWD isolates from WTD expressing homozygous wild-type (116AA) or heterozygous (116AG) PrP, we found that 116AG-prions were conformationally less stable, more sensitive to proteases, with lower seeding activity in cell-free conversion and reduced infectivity. Here, we aimed to understand CWD strain emergence and adaptation. We show that the WTD-116AG isolate contains two different prion strains, distinguished by their host range, biochemical properties, and pathogenesis from WTD-116AA prions (Wisc-1). Serial passages of WTD-116AG prions in tg(CerPrP)1536(+/+) mice overexpressing wild-type deer-PrP(C) revealed two populations of mice with short and long incubation periods, respectively, and remarkably prolonged clinical phase upon inoculation with WTD-116AG prions. Inoculation of serially diluted brain homogenates confirmed the presence of two strains in the 116AG isolate with distinct pathology in the brain. Interestingly, deglycosylation revealed proteinase K-resistant fragments with different electrophoretic mobility in both tg(CerPrP)1536(+/+) mice and Syrian golden hamsters infected with WTD-116AG. Infection of tg60 mice expressing deer S96-PrP with 116AG, but not Wisc-1 prions induced clinical disease. On the contrary, bank voles resisted 116AG prions, but not Wisc-1 infection. Our data indicate that two strains co-existed in the WTD-116AG isolate, expanding the variety of CWD prion strains. We argue that the 116AG isolate does not contain Wisc-1 prions, indicating that the presence of 116G-PrP(C) diverted 116A-PrP(C) from adopting a Wisc-1 structure. This can have important implications for their possible distinct capacities to cross species barriers into both cervids and non-cervids. Public Library of Science 2021-07-26 /pmc/articles/PMC8341689/ /pubmed/34310662 http://dx.doi.org/10.1371/journal.ppat.1009795 Text en © 2021 Hannaoui et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Hannaoui, Samia
Triscott, Elizabeth
Duque Velásquez, Camilo
Chang, Sheng Chun
Arifin, Maria Immaculata
Zemlyankina, Irina
Tang, Xinli
Bollinger, Trent
Wille, Holger
McKenzie, Debbie
Gilch, Sabine
New and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the Prnp gene
title New and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the Prnp gene
title_full New and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the Prnp gene
title_fullStr New and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the Prnp gene
title_full_unstemmed New and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the Prnp gene
title_short New and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the Prnp gene
title_sort new and distinct chronic wasting disease strains associated with cervid polymorphism at codon 116 of the prnp gene
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8341689/
https://www.ncbi.nlm.nih.gov/pubmed/34310662
http://dx.doi.org/10.1371/journal.ppat.1009795
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