Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease

Phenotypic screening has yielded small-molecule inhibitors of prion replication that are effective in vivo against certain prion strains but not others. Here, we sought to test the small molecule anle138b in multiple mouse models of prion disease. In mice inoculated with the RML strain of prions, an...

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Autores principales: Vallabh, Sonia M., Zou, Dan, Pitstick, Rose, O’Moore, Jill, Peters, Janet, Silvius, Derek, Kriz, Jasna, Jackson, Walker S., Carlson, George A., Minikel, Eric Vallabh, Cabin, Deborah E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2023
Materias:
Prions
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9973041/
https://www.ncbi.nlm.nih.gov/pubmed/36651748
http://dx.doi.org/10.1128/jvi.01672-22
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author Vallabh, Sonia M.
Zou, Dan
Pitstick, Rose
O’Moore, Jill
Peters, Janet
Silvius, Derek
Kriz, Jasna
Jackson, Walker S.
Carlson, George A.
Minikel, Eric Vallabh
Cabin, Deborah E.
author_facet Vallabh, Sonia M.
Zou, Dan
Pitstick, Rose
O’Moore, Jill
Peters, Janet
Silvius, Derek
Kriz, Jasna
Jackson, Walker S.
Carlson, George A.
Minikel, Eric Vallabh
Cabin, Deborah E.
author_sort Vallabh, Sonia M.
collection PubMed
description Phenotypic screening has yielded small-molecule inhibitors of prion replication that are effective in vivo against certain prion strains but not others. Here, we sought to test the small molecule anle138b in multiple mouse models of prion disease. In mice inoculated with the RML strain of prions, anle138b doubled survival and durably suppressed astrogliosis measured by live-animal bioluminescence imaging. In knock-in mouse models of the D178N and E200K mutations that cause genetic prion disease, however, we were unable to identify a clear, quantifiable disease endpoint against which to measure therapeutic efficacy. Among untreated animals, the mutations did not impact overall survival, and bioluminescence remained low out to >20 months of age. Vacuolization and PrP deposition were observed in some brain regions in a subset of mutant animals but appeared to be unable to carry the weight of a primary endpoint in a therapeutic study. We conclude that not all animal models of prion disease are suited to well-powered therapeutic efficacy studies, and care should be taken in choosing the models that will support drug development programs. IMPORTANCE There is an urgent need to develop drugs for prion disease, a currently untreatable neurodegenerative disease. In this effort, there is a debate over which animal models can best support a drug development program. While the study of prion disease benefits from excellent animal models because prions naturally afflict many different mammals, different models have different capabilities and limitations. Here, we conducted a therapeutic efficacy study of the drug candidate anle138b in mouse models with two of the most common mutations that cause genetic prion disease. In a more typical model where prions are injected directly into the brain, we found anle138b to be effective. In the genetic models, however, the animals never reached a clear, measurable point of disease onset. We conclude that not all prion disease animal models are ideally suited to drug efficacy studies, and well-defined, quantitative disease metrics should be a priority.
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spelling pubmed-99730412023-03-01 Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease Vallabh, Sonia M. Zou, Dan Pitstick, Rose O’Moore, Jill Peters, Janet Silvius, Derek Kriz, Jasna Jackson, Walker S. Carlson, George A. Minikel, Eric Vallabh Cabin, Deborah E. J Virol Prions Phenotypic screening has yielded small-molecule inhibitors of prion replication that are effective in vivo against certain prion strains but not others. Here, we sought to test the small molecule anle138b in multiple mouse models of prion disease. In mice inoculated with the RML strain of prions, anle138b doubled survival and durably suppressed astrogliosis measured by live-animal bioluminescence imaging. In knock-in mouse models of the D178N and E200K mutations that cause genetic prion disease, however, we were unable to identify a clear, quantifiable disease endpoint against which to measure therapeutic efficacy. Among untreated animals, the mutations did not impact overall survival, and bioluminescence remained low out to >20 months of age. Vacuolization and PrP deposition were observed in some brain regions in a subset of mutant animals but appeared to be unable to carry the weight of a primary endpoint in a therapeutic study. We conclude that not all animal models of prion disease are suited to well-powered therapeutic efficacy studies, and care should be taken in choosing the models that will support drug development programs. IMPORTANCE There is an urgent need to develop drugs for prion disease, a currently untreatable neurodegenerative disease. In this effort, there is a debate over which animal models can best support a drug development program. While the study of prion disease benefits from excellent animal models because prions naturally afflict many different mammals, different models have different capabilities and limitations. Here, we conducted a therapeutic efficacy study of the drug candidate anle138b in mouse models with two of the most common mutations that cause genetic prion disease. In a more typical model where prions are injected directly into the brain, we found anle138b to be effective. In the genetic models, however, the animals never reached a clear, measurable point of disease onset. We conclude that not all prion disease animal models are ideally suited to drug efficacy studies, and well-defined, quantitative disease metrics should be a priority. American Society for Microbiology 2023-01-18 /pmc/articles/PMC9973041/ /pubmed/36651748 http://dx.doi.org/10.1128/jvi.01672-22 Text en Copyright © 2023 Vallabh et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Prions
Vallabh, Sonia M.
Zou, Dan
Pitstick, Rose
O’Moore, Jill
Peters, Janet
Silvius, Derek
Kriz, Jasna
Jackson, Walker S.
Carlson, George A.
Minikel, Eric Vallabh
Cabin, Deborah E.
Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease
title Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease
title_full Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease
title_fullStr Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease
title_full_unstemmed Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease
title_short Therapeutic Trial of anle138b in Mouse Models of Genetic Prion Disease
title_sort therapeutic trial of anle138b in mouse models of genetic prion disease
topic Prions
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9973041/
https://www.ncbi.nlm.nih.gov/pubmed/36651748
http://dx.doi.org/10.1128/jvi.01672-22
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