Q84328 (Q84328): Difference between revisions
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Property / financed by | |||
Property / financed by: European Union / rank | |||
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Property / intervention field: Research and innovation activities in public research centres and centres of competence including networking / rank | |||
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Revision as of 10:51, 31 January 2020
Project in Poland financed by DG Regio
Language | Label | Description | Also known as |
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English | No label defined |
Project in Poland financed by DG Regio |
Statements
3,499,222.0 zloty
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3,499,222.0 zloty
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100.0 percent
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1 October 2018
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30 September 2021
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UNIWERSYTET IM. ADAMA MICKIEWICZA W POZNANIU
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Myotonic Dystrophy (DM) and Fragile X-associated tremor-Ataxia Syndrome (FXTAS) are dominant disorders caused by RNA gain of function of expanded CUG or CGG repeats. Both RNAs may sequester nuclear proteins, and their repeat sequences undergo untypical translation into toxic mono-amino acid peptides. Since the causative molecular target is well defined, DM and FXTAS are highly amenable to the development of RNA targeting therapy. We and others demonstrated that reduction of protein sequestration on toxic CUG repeats using various oligonucleotide-based approaches or small compounds led to promising results in animal models of DM; therefore, now we want to develop similar tools to reduce the effect of FXTAS mutation by targeting RNA with CGG expansion, to reduce its translation rate. We also aim to achieve the gene therapy tool to overexpress the therapeutic proteins which may rescue nuclear proteins from pathogenic sequestration in DM. We are going to study mechanisms of both diseases. (Polish)
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Identifiers
POIR.04.04.00-00-5C0C/17
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