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Grant - Summer 2018 - ALS – Joel Richter, PhD

“There are two outcomes we hope for. One outcome is basic understanding of how toxic peptides are generated from C9orf72. The second outcome – which is some distance in the future – will be to use our knowledge to inhibit the product ion of these toxic peptides and thereby mitigate or delay at least this one form of ALS.”
Joel Richter, Arthur F. Koskinas Chair in Neuroscience, and Fen-Biao Gao, Governor Paul Cellucci Chair in Neuroscience Research, both at the University of Massachusetts Medical School in Worcester, were awarded an MDA Research Grant totaling $300,000 over 3 years to study a potential inhibition of translation of G4C2-containing RNA as a novel therapy for C9orf72-ALS.
Amyotrophic lateral sclerosis (ALS) is a fatal disease caused by motor neuron degeneration and resulting muscle wasting. Most causes of ALS are unknown, but the most commonly known genetic cause is an aberrant C9orf72 gene expansion that leads to the toxic accumulation of dipeptide repeat proteins (DPRs).
Previous collaborative work in Drs. Richter and Gao’s labs has identified regions in C9orf72 RNA that could be blocked by binding to complementary DNA antisense oligonucleotides (AS-ODNs). Such AS-ODNs would inhibit DPR production, thereby slowing or inhibiting disease progression.
Drs. Richter and Gao propose to use human disease neurons in culture and C9orf72 model mice to test the efficacy and specificity of AS-ODNs to inhibit DPR synthesis and mitigate ALS pathophysiology. It’s hoped this work will have a major impact on the clinical treatment of ALS.
Grantee: ALS – Joel Richter, PhD
Grant type: Research Grant
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