MSH3 Polymorphisms and Protein Levels Affect CAG Repeat Instability in Huntington's Disease Mice

Expansions of trinucleotide CAG/CTG repeats in somatic tissues are thought to contribute to ongoing disease progression through an affected individual's life with Huntington's disease or myotonic dystrophy. Broad ranges of repeat instability arise between individuals with expanded repeats,...

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Autores principales: Tomé, Stéphanie, Manley, Kevin, Simard, Jodie P., Clark, Greg W., Slean, Meghan M., Swami, Meera, Shelbourne, Peggy F., Tillier, Elisabeth R. M., Monckton, Darren G., Messer, Anne, Pearson, Christopher E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3585117/
https://www.ncbi.nlm.nih.gov/pubmed/23468640
http://dx.doi.org/10.1371/journal.pgen.1003280
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author Tomé, Stéphanie
Manley, Kevin
Simard, Jodie P.
Clark, Greg W.
Slean, Meghan M.
Swami, Meera
Shelbourne, Peggy F.
Tillier, Elisabeth R. M.
Monckton, Darren G.
Messer, Anne
Pearson, Christopher E.
author_facet Tomé, Stéphanie
Manley, Kevin
Simard, Jodie P.
Clark, Greg W.
Slean, Meghan M.
Swami, Meera
Shelbourne, Peggy F.
Tillier, Elisabeth R. M.
Monckton, Darren G.
Messer, Anne
Pearson, Christopher E.
author_sort Tomé, Stéphanie
collection PubMed
description Expansions of trinucleotide CAG/CTG repeats in somatic tissues are thought to contribute to ongoing disease progression through an affected individual's life with Huntington's disease or myotonic dystrophy. Broad ranges of repeat instability arise between individuals with expanded repeats, suggesting the existence of modifiers of repeat instability. Mice with expanded CAG/CTG repeats show variable levels of instability depending upon mouse strain. However, to date the genetic modifiers underlying these differences have not been identified. We show that in liver and striatum the R6/1 Huntington's disease (HD) (CAG)∼100 transgene, when present in a congenic C57BL/6J (B6) background, incurred expansion-biased repeat mutations, whereas the repeat was stable in a congenic BALB/cByJ (CBy) background. Reciprocal congenic mice revealed the Msh3 gene as the determinant for the differences in repeat instability. Expansion bias was observed in congenic mice homozygous for the B6 Msh3 gene on a CBy background, while the CAG tract was stabilized in congenics homozygous for the CBy Msh3 gene on a B6 background. The CAG stabilization was as dramatic as genetic deficiency of Msh2. The B6 and CBy Msh3 genes had identical promoters but differed in coding regions and showed strikingly different protein levels. B6 MSH3 variant protein is highly expressed and associated with CAG expansions, while the CBy MSH3 variant protein is expressed at barely detectable levels, associating with CAG stability. The DHFR protein, which is divergently transcribed from a promoter shared by the Msh3 gene, did not show varied levels between mouse strains. Thus, naturally occurring MSH3 protein polymorphisms are modifiers of CAG repeat instability, likely through variable MSH3 protein stability. Since evidence supports that somatic CAG instability is a modifier and predictor of disease, our data are consistent with the hypothesis that variable levels of CAG instability associated with polymorphisms of DNA repair genes may have prognostic implications for various repeat-associated diseases.
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spelling pubmed-35851172013-03-06 MSH3 Polymorphisms and Protein Levels Affect CAG Repeat Instability in Huntington's Disease Mice Tomé, Stéphanie Manley, Kevin Simard, Jodie P. Clark, Greg W. Slean, Meghan M. Swami, Meera Shelbourne, Peggy F. Tillier, Elisabeth R. M. Monckton, Darren G. Messer, Anne Pearson, Christopher E. PLoS Genet Research Article Expansions of trinucleotide CAG/CTG repeats in somatic tissues are thought to contribute to ongoing disease progression through an affected individual's life with Huntington's disease or myotonic dystrophy. Broad ranges of repeat instability arise between individuals with expanded repeats, suggesting the existence of modifiers of repeat instability. Mice with expanded CAG/CTG repeats show variable levels of instability depending upon mouse strain. However, to date the genetic modifiers underlying these differences have not been identified. We show that in liver and striatum the R6/1 Huntington's disease (HD) (CAG)∼100 transgene, when present in a congenic C57BL/6J (B6) background, incurred expansion-biased repeat mutations, whereas the repeat was stable in a congenic BALB/cByJ (CBy) background. Reciprocal congenic mice revealed the Msh3 gene as the determinant for the differences in repeat instability. Expansion bias was observed in congenic mice homozygous for the B6 Msh3 gene on a CBy background, while the CAG tract was stabilized in congenics homozygous for the CBy Msh3 gene on a B6 background. The CAG stabilization was as dramatic as genetic deficiency of Msh2. The B6 and CBy Msh3 genes had identical promoters but differed in coding regions and showed strikingly different protein levels. B6 MSH3 variant protein is highly expressed and associated with CAG expansions, while the CBy MSH3 variant protein is expressed at barely detectable levels, associating with CAG stability. The DHFR protein, which is divergently transcribed from a promoter shared by the Msh3 gene, did not show varied levels between mouse strains. Thus, naturally occurring MSH3 protein polymorphisms are modifiers of CAG repeat instability, likely through variable MSH3 protein stability. Since evidence supports that somatic CAG instability is a modifier and predictor of disease, our data are consistent with the hypothesis that variable levels of CAG instability associated with polymorphisms of DNA repair genes may have prognostic implications for various repeat-associated diseases. Public Library of Science 2013-02-28 /pmc/articles/PMC3585117/ /pubmed/23468640 http://dx.doi.org/10.1371/journal.pgen.1003280 Text en © 2013 Tomé et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Tomé, Stéphanie
Manley, Kevin
Simard, Jodie P.
Clark, Greg W.
Slean, Meghan M.
Swami, Meera
Shelbourne, Peggy F.
Tillier, Elisabeth R. M.
Monckton, Darren G.
Messer, Anne
Pearson, Christopher E.
MSH3 Polymorphisms and Protein Levels Affect CAG Repeat Instability in Huntington's Disease Mice
title MSH3 Polymorphisms and Protein Levels Affect CAG Repeat Instability in Huntington's Disease Mice
title_full MSH3 Polymorphisms and Protein Levels Affect CAG Repeat Instability in Huntington's Disease Mice
title_fullStr MSH3 Polymorphisms and Protein Levels Affect CAG Repeat Instability in Huntington's Disease Mice
title_full_unstemmed MSH3 Polymorphisms and Protein Levels Affect CAG Repeat Instability in Huntington's Disease Mice
title_short MSH3 Polymorphisms and Protein Levels Affect CAG Repeat Instability in Huntington's Disease Mice
title_sort msh3 polymorphisms and protein levels affect cag repeat instability in huntington's disease mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3585117/
https://www.ncbi.nlm.nih.gov/pubmed/23468640
http://dx.doi.org/10.1371/journal.pgen.1003280
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