Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm

Prion diseases are transmissible neurodegenerative disorders that affect mammals, including humans. The central molecular event is the conversion of cellular prion glycoprotein, PrP(C), into a plethora of assemblies, PrP(Sc), associated with disease. Distinct phenotypes of disease led to the concept...

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Autores principales: Cortez, Leonardo M., Nemani, Satish K., Duque Velásquez, Camilo, Sriraman, Aishwarya, Wang, YongLiang, Wille, Holger, McKenzie, Debbie, Sim, Valerie L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8270404/
https://www.ncbi.nlm.nih.gov/pubmed/34181702
http://dx.doi.org/10.1371/journal.ppat.1009703
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author Cortez, Leonardo M.
Nemani, Satish K.
Duque Velásquez, Camilo
Sriraman, Aishwarya
Wang, YongLiang
Wille, Holger
McKenzie, Debbie
Sim, Valerie L.
author_facet Cortez, Leonardo M.
Nemani, Satish K.
Duque Velásquez, Camilo
Sriraman, Aishwarya
Wang, YongLiang
Wille, Holger
McKenzie, Debbie
Sim, Valerie L.
author_sort Cortez, Leonardo M.
collection PubMed
description Prion diseases are transmissible neurodegenerative disorders that affect mammals, including humans. The central molecular event is the conversion of cellular prion glycoprotein, PrP(C), into a plethora of assemblies, PrP(Sc), associated with disease. Distinct phenotypes of disease led to the concept of prion strains, which are associated with distinct PrP(Sc) structures. However, the degree to which intra- and inter-strain PrP(Sc) heterogeneity contributes to disease pathogenesis remains unclear. Addressing this question requires the precise isolation and characterization of all PrP(Sc) subpopulations from the prion-infected brains. Until now, this has been challenging. We used asymmetric-flow field-flow fractionation (AF4) to isolate all PrP(Sc) subpopulations from brains of hamsters infected with three prion strains: Hyper (HY) and 263K, which produce almost identical phenotypes, and Drowsy (DY), a strain with a distinct presentation. In-line dynamic and multi-angle light scattering (DLS/MALS) data provided accurate measurements of particle sizes and estimation of the shape and number of PrP(Sc) particles. We found that each strain had a continuum of PrP(Sc) assemblies, with strong correlation between PrP(Sc) quaternary structure and phenotype. HY and 263K were enriched with large, protease-resistant PrP(Sc) aggregates, whereas DY consisted primarily of smaller, more protease-sensitive aggregates. For all strains, a transition from protease-sensitive to protease-resistant PrP(Sc) took place at a hydrodynamic radius (R(h)) of 15 nm and was accompanied by a change in glycosylation and seeding activity. Our results show that the combination of AF4 with in-line MALS/DLS is a powerful tool for analyzing PrP(Sc) subpopulations and demonstrate that while PrP(Sc) quaternary structure is a major contributor to PrP(Sc) structural heterogeneity, a fundamental change, likely in secondary/tertiary structure, prevents PrP(Sc) particles from maintaining proteinase K resistance below an R(h) of 15 nm, regardless of strain. This results in two biochemically distinctive subpopulations, the proportion, seeding activity, and stability of which correlate with prion strain phenotype.
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spelling pubmed-82704042021-07-20 Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm Cortez, Leonardo M. Nemani, Satish K. Duque Velásquez, Camilo Sriraman, Aishwarya Wang, YongLiang Wille, Holger McKenzie, Debbie Sim, Valerie L. PLoS Pathog Research Article Prion diseases are transmissible neurodegenerative disorders that affect mammals, including humans. The central molecular event is the conversion of cellular prion glycoprotein, PrP(C), into a plethora of assemblies, PrP(Sc), associated with disease. Distinct phenotypes of disease led to the concept of prion strains, which are associated with distinct PrP(Sc) structures. However, the degree to which intra- and inter-strain PrP(Sc) heterogeneity contributes to disease pathogenesis remains unclear. Addressing this question requires the precise isolation and characterization of all PrP(Sc) subpopulations from the prion-infected brains. Until now, this has been challenging. We used asymmetric-flow field-flow fractionation (AF4) to isolate all PrP(Sc) subpopulations from brains of hamsters infected with three prion strains: Hyper (HY) and 263K, which produce almost identical phenotypes, and Drowsy (DY), a strain with a distinct presentation. In-line dynamic and multi-angle light scattering (DLS/MALS) data provided accurate measurements of particle sizes and estimation of the shape and number of PrP(Sc) particles. We found that each strain had a continuum of PrP(Sc) assemblies, with strong correlation between PrP(Sc) quaternary structure and phenotype. HY and 263K were enriched with large, protease-resistant PrP(Sc) aggregates, whereas DY consisted primarily of smaller, more protease-sensitive aggregates. For all strains, a transition from protease-sensitive to protease-resistant PrP(Sc) took place at a hydrodynamic radius (R(h)) of 15 nm and was accompanied by a change in glycosylation and seeding activity. Our results show that the combination of AF4 with in-line MALS/DLS is a powerful tool for analyzing PrP(Sc) subpopulations and demonstrate that while PrP(Sc) quaternary structure is a major contributor to PrP(Sc) structural heterogeneity, a fundamental change, likely in secondary/tertiary structure, prevents PrP(Sc) particles from maintaining proteinase K resistance below an R(h) of 15 nm, regardless of strain. This results in two biochemically distinctive subpopulations, the proportion, seeding activity, and stability of which correlate with prion strain phenotype. Public Library of Science 2021-06-28 /pmc/articles/PMC8270404/ /pubmed/34181702 http://dx.doi.org/10.1371/journal.ppat.1009703 Text en © 2021 Cortez 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
Cortez, Leonardo M.
Nemani, Satish K.
Duque Velásquez, Camilo
Sriraman, Aishwarya
Wang, YongLiang
Wille, Holger
McKenzie, Debbie
Sim, Valerie L.
Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm
title Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm
title_full Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm
title_fullStr Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm
title_full_unstemmed Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm
title_short Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm
title_sort asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8270404/
https://www.ncbi.nlm.nih.gov/pubmed/34181702
http://dx.doi.org/10.1371/journal.ppat.1009703
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