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Open-Label Sulforaphane Trial in FMR1 Premutation Carriers with Fragile-X-Associated Tremor and Ataxia Syndrome (FXTAS)
- Santos, Ellery;
- Clark, Courtney;
- Biag, Hazel Maridith B;
- Tang, Si Jie;
- Kim, Kyoungmi;
- Ponzini, Matthew D;
- Schneider, Andrea;
- Giulivi, Cecilia;
- Montanaro, Federica Alice Maria;
- Gipe, Jesse Tran-Emilia;
- Dayton, Jacquelyn;
- Randol, Jamie L;
- Yao, Pamela J;
- Manolopoulos, Apostolos;
- Kapogiannis, Dimitrios;
- Hwang, Ye Hyun;
- Hagerman, Paul;
- Hagerman, Randi;
- Tassone, Flora
- et al.
Published Web Location
https://doi.org/10.3390/cells12242773Abstract
Fragile X (FMR1) premutation is a common mutation that affects about 1 in 200 females and 1 in 450 males and can lead to the development of fragile-X-associated tremor/ataxia syndrome (FXTAS). Although there is no targeted, proven treatment for FXTAS, research suggests that sulforaphane, an antioxidant present in cruciferous vegetables, can enhance mitochondrial function and maintain redox balance in the dermal fibroblasts of individuals with FXTAS, potentially leading to improved cognitive function. In a 24-week open-label trial involving 15 adults aged 60-88 with FXTAS, 11 participants successfully completed the study, demonstrating the safety and tolerability of sulforaphane. Clinical outcomes and biomarkers were measured to elucidate the effects of sulforaphane. While there were nominal improvements in multiple clinical measures, they were not significantly different after correction for multiple comparisons. PBMC energetic measures showed that the level of citrate synthase was higher after sulforaphane treatment, resulting in lower ATP production. The ratio of complex I to complex II showed positive correlations with the MoCA and BDS scores. Several mitochondrial biomarkers showed increased activity and quantity and were correlated with clinical improvements.
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