Local protein synthesis is vital for neuronal function, but its dysregulation in neurodegenerative diseases remains poorly defined. Here we applied spatial transcriptomics to adult mouse motor nerve axons and cell bodies to enable subcellular mapping. Among transcripts found in mature axons, the most enriched biological process is protein translation, and localization of translation machinery was confirmed using multiplexed single-molecule spatial transcriptomics combined with immunofluorescence. Amyotrophic lateral sclerosis (ALS)-associated mutations in the RNA-binding protein fused in sarcoma (FUS), which suppress local translation, disrupt the compartment-specific RNA signatures, including components of the translation machinery. In particular, eukaryotic initiation factor 5a (Eif5a), a translation factor involved in elongation and termination, is found to be locally impaired in mutant FUS axons with reduced levels of its active hypusinated form. Axon-specific treatment with polyamine spermidine restores Eif5a hypusination and ameliorates mutant FUS-dependent neuronal defects, including suppression of local protein synthesis. Finally, in vivo spermidine treatment reduces ALS-related toxicity in mutant FUS and TDP-43 Drosophila models, which may have implications for therapy development.
Axonal Eif5a hypusination controls local translation and mitigates defects in FUS-ALS.
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作者:Piol Diana, Khalil Bilal, Robberechts Tessa, Killian Theo, Georgopoulou Maria, Partel Gabriele, Wouters David, Hecker Nikolai, Tziortzouda Paraskevi, Verresen Yana, Corthout Nikky, Kint Sam, Vandereyken Katy, Van Damme Philip, Voet Thierry, Davie Kristofer, Poovathingal Suresh, Van Den Bosch Ludo, Aerts Stein, Sifrim Alejandro, Da Cruz Sandrine
| 期刊: | Nature Neuroscience | 影响因子: | 20.000 |
| 时间: | 2026 | 起止号: | 2026 Jan;29(1):53-66 |
| doi: | 10.1038/s41593-025-02101-2 | ||
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