Molecular, Physiological, and Motor Performance Defects in DMSXL Mice Carrying >1,000 CTG Repeats from the Human DM1 Locus

Myotonic dystrophy type 1 (DM1) is caused by an unstable CTG repeat expansion in the 3′UTR of the DM protein kinase (DMPK) gene. DMPK transcripts carrying CUG expansions form nuclear foci and affect splicing regulation of various RNA transcripts. Furthermore, bidirectional transcription over the DMP...

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Autores principales: Huguet, Aline, Medja, Fadia, Nicole, Annie, Vignaud, Alban, Guiraud-Dogan, Céline, Ferry, Arnaud, Decostre, Valérie, Hogrel, Jean-Yves, Metzger, Friedrich, Hoeflich, Andreas, Baraibar, Martin, Gomes-Pereira, Mário, Puymirat, Jack, Bassez, Guillaume, Furling, Denis, Munnich, Arnold, Gourdon, Geneviève
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3510028/
https://www.ncbi.nlm.nih.gov/pubmed/23209425
http://dx.doi.org/10.1371/journal.pgen.1003043
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author Huguet, Aline
Medja, Fadia
Nicole, Annie
Vignaud, Alban
Guiraud-Dogan, Céline
Ferry, Arnaud
Decostre, Valérie
Hogrel, Jean-Yves
Metzger, Friedrich
Hoeflich, Andreas
Baraibar, Martin
Gomes-Pereira, Mário
Puymirat, Jack
Bassez, Guillaume
Furling, Denis
Munnich, Arnold
Gourdon, Geneviève
author_facet Huguet, Aline
Medja, Fadia
Nicole, Annie
Vignaud, Alban
Guiraud-Dogan, Céline
Ferry, Arnaud
Decostre, Valérie
Hogrel, Jean-Yves
Metzger, Friedrich
Hoeflich, Andreas
Baraibar, Martin
Gomes-Pereira, Mário
Puymirat, Jack
Bassez, Guillaume
Furling, Denis
Munnich, Arnold
Gourdon, Geneviève
author_sort Huguet, Aline
collection PubMed
description Myotonic dystrophy type 1 (DM1) is caused by an unstable CTG repeat expansion in the 3′UTR of the DM protein kinase (DMPK) gene. DMPK transcripts carrying CUG expansions form nuclear foci and affect splicing regulation of various RNA transcripts. Furthermore, bidirectional transcription over the DMPK gene and non-conventional RNA translation of repeated transcripts have been described in DM1. It is clear now that this disease may involve multiple pathogenic pathways including changes in gene expression, RNA stability and splicing regulation, protein translation, and micro–RNA metabolism. We previously generated transgenic mice with 45-kb of the DM1 locus and >300 CTG repeats (DM300 mice). After successive breeding and a high level of CTG repeat instability, we obtained transgenic mice carrying >1,000 CTG (DMSXL mice). Here we described for the first time the expression pattern of the DMPK sense transcripts in DMSXL and human tissues. Interestingly, we also demonstrate that DMPK antisense transcripts are expressed in various DMSXL and human tissues, and that both sense and antisense transcripts accumulate in independent nuclear foci that do not co-localize together. Molecular features of DM1-associated RNA toxicity in DMSXL mice (such as foci accumulation and mild missplicing), were associated with high mortality, growth retardation, and muscle defects (abnormal histopathology, reduced muscle strength, and lower motor performances). We have found that lower levels of IGFBP-3 may contribute to DMSXL growth retardation, while increased proteasome activity may affect muscle function. These data demonstrate that the human DM1 locus carrying very large expansions induced a variety of molecular and physiological defects in transgenic mice, reflecting DM1 to a certain extent. As a result, DMSXL mice provide an animal tool to decipher various aspects of the disease mechanisms. In addition, these mice can be used to test the preclinical impact of systemic therapeutic strategies on molecular and physiological phenotypes.
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spelling pubmed-35100282012-12-03 Molecular, Physiological, and Motor Performance Defects in DMSXL Mice Carrying >1,000 CTG Repeats from the Human DM1 Locus Huguet, Aline Medja, Fadia Nicole, Annie Vignaud, Alban Guiraud-Dogan, Céline Ferry, Arnaud Decostre, Valérie Hogrel, Jean-Yves Metzger, Friedrich Hoeflich, Andreas Baraibar, Martin Gomes-Pereira, Mário Puymirat, Jack Bassez, Guillaume Furling, Denis Munnich, Arnold Gourdon, Geneviève PLoS Genet Research Article Myotonic dystrophy type 1 (DM1) is caused by an unstable CTG repeat expansion in the 3′UTR of the DM protein kinase (DMPK) gene. DMPK transcripts carrying CUG expansions form nuclear foci and affect splicing regulation of various RNA transcripts. Furthermore, bidirectional transcription over the DMPK gene and non-conventional RNA translation of repeated transcripts have been described in DM1. It is clear now that this disease may involve multiple pathogenic pathways including changes in gene expression, RNA stability and splicing regulation, protein translation, and micro–RNA metabolism. We previously generated transgenic mice with 45-kb of the DM1 locus and >300 CTG repeats (DM300 mice). After successive breeding and a high level of CTG repeat instability, we obtained transgenic mice carrying >1,000 CTG (DMSXL mice). Here we described for the first time the expression pattern of the DMPK sense transcripts in DMSXL and human tissues. Interestingly, we also demonstrate that DMPK antisense transcripts are expressed in various DMSXL and human tissues, and that both sense and antisense transcripts accumulate in independent nuclear foci that do not co-localize together. Molecular features of DM1-associated RNA toxicity in DMSXL mice (such as foci accumulation and mild missplicing), were associated with high mortality, growth retardation, and muscle defects (abnormal histopathology, reduced muscle strength, and lower motor performances). We have found that lower levels of IGFBP-3 may contribute to DMSXL growth retardation, while increased proteasome activity may affect muscle function. These data demonstrate that the human DM1 locus carrying very large expansions induced a variety of molecular and physiological defects in transgenic mice, reflecting DM1 to a certain extent. As a result, DMSXL mice provide an animal tool to decipher various aspects of the disease mechanisms. In addition, these mice can be used to test the preclinical impact of systemic therapeutic strategies on molecular and physiological phenotypes. Public Library of Science 2012-11-29 /pmc/articles/PMC3510028/ /pubmed/23209425 http://dx.doi.org/10.1371/journal.pgen.1003043 Text en © 2012 Huguet 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
Huguet, Aline
Medja, Fadia
Nicole, Annie
Vignaud, Alban
Guiraud-Dogan, Céline
Ferry, Arnaud
Decostre, Valérie
Hogrel, Jean-Yves
Metzger, Friedrich
Hoeflich, Andreas
Baraibar, Martin
Gomes-Pereira, Mário
Puymirat, Jack
Bassez, Guillaume
Furling, Denis
Munnich, Arnold
Gourdon, Geneviève
Molecular, Physiological, and Motor Performance Defects in DMSXL Mice Carrying >1,000 CTG Repeats from the Human DM1 Locus
title Molecular, Physiological, and Motor Performance Defects in DMSXL Mice Carrying >1,000 CTG Repeats from the Human DM1 Locus
title_full Molecular, Physiological, and Motor Performance Defects in DMSXL Mice Carrying >1,000 CTG Repeats from the Human DM1 Locus
title_fullStr Molecular, Physiological, and Motor Performance Defects in DMSXL Mice Carrying >1,000 CTG Repeats from the Human DM1 Locus
title_full_unstemmed Molecular, Physiological, and Motor Performance Defects in DMSXL Mice Carrying >1,000 CTG Repeats from the Human DM1 Locus
title_short Molecular, Physiological, and Motor Performance Defects in DMSXL Mice Carrying >1,000 CTG Repeats from the Human DM1 Locus
title_sort molecular, physiological, and motor performance defects in dmsxl mice carrying >1,000 ctg repeats from the human dm1 locus
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3510028/
https://www.ncbi.nlm.nih.gov/pubmed/23209425
http://dx.doi.org/10.1371/journal.pgen.1003043
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