Motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the B6.Htt(Q111/+) model of Huntington’s disease

We investigated the appearance and progression of disease-relevant signs in the B6.Htt(Q111/+) mouse, a genetically precise model of the mutation that causes Huntington’s disease (HD). We find that B6.Htt(Q111/+) mice are healthy, show no overt signs of central or peripheral inflammation, and no gro...

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Autores principales: Bragg, Robert M., Coffey, Sydney R., Weston, Rory M., Ament, Seth A., Cantle, Jeffrey P., Minnig, Shawn, Funk, Cory C., Shuttleworth, Dominic D., Woods, Emily L., Sullivan, Bonnie R., Jones, Lindsey, Glickenhaus, Anne, Anderson, John S., Anderson, Michael D., Dunnett, Stephen B., Wheeler, Vanessa C., MacDonald, Marcy E., Brooks, Simon P., Price, Nathan D., Carroll, Jeffrey B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2017
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5296868/
https://www.ncbi.nlm.nih.gov/pubmed/28176805
http://dx.doi.org/10.1038/srep41570
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author Bragg, Robert M.
Coffey, Sydney R.
Weston, Rory M.
Ament, Seth A.
Cantle, Jeffrey P.
Minnig, Shawn
Funk, Cory C.
Shuttleworth, Dominic D.
Woods, Emily L.
Sullivan, Bonnie R.
Jones, Lindsey
Glickenhaus, Anne
Anderson, John S.
Anderson, Michael D.
Dunnett, Stephen B.
Wheeler, Vanessa C.
MacDonald, Marcy E.
Brooks, Simon P.
Price, Nathan D.
Carroll, Jeffrey B.
author_facet Bragg, Robert M.
Coffey, Sydney R.
Weston, Rory M.
Ament, Seth A.
Cantle, Jeffrey P.
Minnig, Shawn
Funk, Cory C.
Shuttleworth, Dominic D.
Woods, Emily L.
Sullivan, Bonnie R.
Jones, Lindsey
Glickenhaus, Anne
Anderson, John S.
Anderson, Michael D.
Dunnett, Stephen B.
Wheeler, Vanessa C.
MacDonald, Marcy E.
Brooks, Simon P.
Price, Nathan D.
Carroll, Jeffrey B.
author_sort Bragg, Robert M.
collection PubMed
description We investigated the appearance and progression of disease-relevant signs in the B6.Htt(Q111/+) mouse, a genetically precise model of the mutation that causes Huntington’s disease (HD). We find that B6.Htt(Q111/+) mice are healthy, show no overt signs of central or peripheral inflammation, and no gross motor impairment as late as 12 months of age. Behaviorally, we find that 4–9 month old B6.Htt(Q111/+) mice have normal activity levels and show no clear signs of anxiety or depression, but do show clear signs of reduced motivation. The neuronal density, neuronal size, synaptic density and number of glia is normal in B6.Htt(Q111/+) striatum, the most vulnerable brain region in HD, up to 12 months of age. Despite this preservation of the synaptic and cellular composition of the striatum, we observe clear progressive, striatal-specific transcriptional dysregulation and accumulation of neuronal intranuclear inclusions (NIIs). Simulation studies suggest these molecular endpoints are sufficiently robust for future preclinical studies, and that B6.Htt(Q111/+) mice are a useful tool for modeling disease-modifying or neuroprotective strategies for disease processes before the onset of overt phenotypes.
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spelling pubmed-52968682017-02-13 Motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the B6.Htt(Q111/+) model of Huntington’s disease Bragg, Robert M. Coffey, Sydney R. Weston, Rory M. Ament, Seth A. Cantle, Jeffrey P. Minnig, Shawn Funk, Cory C. Shuttleworth, Dominic D. Woods, Emily L. Sullivan, Bonnie R. Jones, Lindsey Glickenhaus, Anne Anderson, John S. Anderson, Michael D. Dunnett, Stephen B. Wheeler, Vanessa C. MacDonald, Marcy E. Brooks, Simon P. Price, Nathan D. Carroll, Jeffrey B. Sci Rep Article We investigated the appearance and progression of disease-relevant signs in the B6.Htt(Q111/+) mouse, a genetically precise model of the mutation that causes Huntington’s disease (HD). We find that B6.Htt(Q111/+) mice are healthy, show no overt signs of central or peripheral inflammation, and no gross motor impairment as late as 12 months of age. Behaviorally, we find that 4–9 month old B6.Htt(Q111/+) mice have normal activity levels and show no clear signs of anxiety or depression, but do show clear signs of reduced motivation. The neuronal density, neuronal size, synaptic density and number of glia is normal in B6.Htt(Q111/+) striatum, the most vulnerable brain region in HD, up to 12 months of age. Despite this preservation of the synaptic and cellular composition of the striatum, we observe clear progressive, striatal-specific transcriptional dysregulation and accumulation of neuronal intranuclear inclusions (NIIs). Simulation studies suggest these molecular endpoints are sufficiently robust for future preclinical studies, and that B6.Htt(Q111/+) mice are a useful tool for modeling disease-modifying or neuroprotective strategies for disease processes before the onset of overt phenotypes. Nature Publishing Group 2017-02-08 /pmc/articles/PMC5296868/ /pubmed/28176805 http://dx.doi.org/10.1038/srep41570 Text en Copyright © 2017, The Author(s) http://creativecommons.org/licenses/by/4.0/ This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/
spellingShingle Article
Bragg, Robert M.
Coffey, Sydney R.
Weston, Rory M.
Ament, Seth A.
Cantle, Jeffrey P.
Minnig, Shawn
Funk, Cory C.
Shuttleworth, Dominic D.
Woods, Emily L.
Sullivan, Bonnie R.
Jones, Lindsey
Glickenhaus, Anne
Anderson, John S.
Anderson, Michael D.
Dunnett, Stephen B.
Wheeler, Vanessa C.
MacDonald, Marcy E.
Brooks, Simon P.
Price, Nathan D.
Carroll, Jeffrey B.
Motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the B6.Htt(Q111/+) model of Huntington’s disease
title Motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the B6.Htt(Q111/+) model of Huntington’s disease
title_full Motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the B6.Htt(Q111/+) model of Huntington’s disease
title_fullStr Motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the B6.Htt(Q111/+) model of Huntington’s disease
title_full_unstemmed Motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the B6.Htt(Q111/+) model of Huntington’s disease
title_short Motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the B6.Htt(Q111/+) model of Huntington’s disease
title_sort motivational, proteostatic and transcriptional deficits precede synapse loss, gliosis and neurodegeneration in the b6.htt(q111/+) model of huntington’s disease
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5296868/
https://www.ncbi.nlm.nih.gov/pubmed/28176805
http://dx.doi.org/10.1038/srep41570
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