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Targeting the Mitoribosome to Treat Mitochondrial Myopathies
The central problem of this application is to test the efficacy of tetracyclines, among them doxycycline, to treat mitochondrial myopathies. There are no cures for these diseases and treatments are more often palliative and include vitamins and supplements, nutritional manipulations, and exercise. Mitochondrial myopathies result from mutations in mitochondrial or nuclear DNA that cause failures in energetic and metabolic function. We have recently developed chemical screen platforms to discover drugs that rescue pathologies caused by human mitochondrial disease mutations. Importantly, we have identified that certain antibiotics, such as doxycycline, that are FDA approved and used in the clinic, are effective in cellular and mouse pre-clinical models of mitochondrial diseases. However, whether these antibiotics are effective in mitochondrial myopathies, and how they work are unknown. In this application (1) we will investigate the efficacy of doxycycline in a mouse pre-clinical model of mitochondrial myopathy, and (2) we will use CRISPR modifying genetic screens to discover how these antibiotics work. The final goal is to provide scientific based support for the use of these antibiotics, or newly identified targets, to treat mitochondrial myopathies.
Grantee: Pere Puigserver
Grant type: Research Grant
Award total: $300,000.00
Institution: Dana-Farber Cancer Institute
Country: United States