ALS/FTD-Linked Mutation in FUS Suppresses Intra-axonal Protein Synthesis and Drives Disease Without Nuclear Loss-of-Function of FUS
- López-Erauskin, Jone
- Tadokoro, Takahiro
- Baughn, Michael W.
- Myers, Brian
- McAlonis-Downes, Melissa
- Chillon-Marinas, Carlos
- Asiaban, Joshua N.
- Artates, Jonathan
- Bui, Anh T.
- Vetto, Anne P.
- Lee, Sandra K.
- Le, Ai Vy
- Sun, Ying
- Jambeau, Mélanie
- Boubaker, Jihane
- Swing, Deborah
- Qiu, Jinsong
- Hicks, Geoffrey G.
- Ouyang, Zhengyu
- Fu, Xiang-Dong
- Tessarollo, Lino
- Ling, Shuo-Chien
- Parone, Philippe A.
- Shaw, Christopher E.
- Marsala, Martin
- Lagier-Tourenne, Clotilde
- Cleveland, Don W.
- Da Cruz, Sandrine
DOIAbstract
Summary Through the generation of humanized FUS mice expressing full-length human FUS, we identify that when expressed at near endogenous murine FUS levels, both wild-type and ALS-causing and frontotemporal dementia (FTD)-causing mutations complement the essential function(s) of murine FUS. Replacement of murine FUS with mutant, but not wild-type, human FUS causes stress-mediated induction of chaperones, decreased expression of ion channels and transporters essential for synaptic function, and reduced synaptic activity without loss of nuclear FUS or its cytoplasmic aggregation. Most strikingly, accumulation of mutant human FUS is shown to activate an integrated stress response and to inhibit local, intra-axonal protein synthesis in hippocam...
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