Impact of the chromatin environment on the CTG repeat instability involved in myotonic dystrophy type 1

Objective

Since the identification of unstable trinucleotide repeats (TNRs) as the genetic cause of human neurological diseases, many studies have tried to unravel the mechanisms of repeat expansion. MSH2 and MSH3, DNA mismatch repair proteins, modify expansion in transgenic mice. Circumstantial evidence suggests that cis-elements surrounding the repeats modulate their instability. However, a detailed analysis of the relationship between chromatin environment and trinucleotide repeat instability is lacking. I will address this issue using transgenic mice that show the highest levels of CTG repeat instability observed in mice thus far. These animals carry long human genomic sequences spanning the DM1 locus containing normal or expanded CTG repeats. I will compare the chromatin status around the repeat in different tissues, showing different degrees of instability, throughout development. DM1 transgenic mice lacking MSH2 display predominantly repeat contractions, providing a unique tool to unravel the contraction mechanisms. This will yield important clues towards the development of new therapeutic approaches, possibly by inducing contractions, as the increase in trinucleotide somatic instability with age is thought to contribute to disease progression. The new insights will also be invaluable for halting intergenerational instability, which leads to new and often more severe cases in the next generation. Therefore, the chromatin studies will be extended to Msh2-/- tissues. Double strand breaks (DSBs) may form at CTG repeats and might be repaired via recombination processes, The formation of gamma-H2AX foci, a signature of DSB formation, will be examined at the DM1 locus, to test whether contractions arise as a consequence of DSBs and recombination in Msh2-/- mice. Since the many different TNR diseases share important genetic properties, increased understanding of the CTG repeat instability mechanisms will undoubtedly be beneficial for this group of disorders.

Fields of science (EuroSciVoc)

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• natural sciences biological sciences genetics DNA
• natural sciences biological sciences biochemistry biomolecules proteins

Programme(s)

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• FP7-PEOPLE - Specific programme "People" implementing the Seventh Framework Programme of the European Community for research, technological development and demonstration activities (2007 to 2013)

Topic(s)

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• FP7-PEOPLE-2009-IEF - Marie Curie Action: "Intra-European Fellowships for Career Development"

Call for proposal

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FP7-PEOPLE-2009-IEF
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Funding Scheme

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MC-IEF - Intra-European Fellowships (IEF)

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