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Grant - Winter 2019 - DM - Matthew Disney, PhD

"We hope to establish a new paradigm in drug design in which one can target RNA with small molecules and use small molecules to destroy toxic RNAs."
Matthew Disney, PhD, professor of Chemistry at The Scripps Research Institute, Florida, was awarded an MDA research grant totaling $300,000 over three years to develop and optimize small molecules targeting the RNA repeats in myotonic dystrophy type 2 (DM2).
DM2 is a neuromuscular disease that causes wasting of many muscles, as well as cardiac disease and cataracts. It is caused by an abnormally expanded section in a gene on chromosome 3 called ZNF9. The DM2 repeat expansion is present in the highest amounts in muscle and heart tissue. This repeat expansion leads to aggregates of RNA inside the cell that become toxic in DM2, effectively sequestering a protein that normally regulates how RNA is spliced (processed). Inactivating this RNA-processing protein has been shown to cause many of the symptoms associated with myotonic dystrophy.
In this work, Dr. Disney will focus on inactivating and eliminating the repeat expansion. He and his team previously designed small molecules that bind to and inactivate the toxic RNA in cellular models. They will build off that work to optimize their small-molecule compounds to both bind the RNA as well cleave it, thus ridding the cell of it. Specifically, he will conduct medicinal chemistry on lead compounds, assemble them into dimers to increase potency and selectivity, give the dimers the ability to cleave the RNA, and test them both in vitro (in patient-derived cells) and in animal models.
https://doi.org/10.55762/pc.gr.84545
Grantee: DM - Matthew Disney, PhD
Grant type: Research Grant
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