Mutation of the ALS-/FTD-Associated RNA-Binding Protein FUS Affects Axonal Development.
Accepted version
Peer-reviewed
Repository URI
Repository DOI
Change log
Authors
Abstract
Aberrant condensation and localization of the RNA-binding protein (RBP) fused in sarcoma (FUS) occur in variants of amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). Changes in RBP function are commonly associated with changes in axonal cytoskeletal organization and branching in neurodevelopmental disorders. Here, we asked whether branching defects also occur in vivo in a model of FUS-associated disease. We use two reported Xenopus models of ALS/FTD (of either sex), the ALS-associated mutant FUS(P525L) and a mimic of hypomethylated FUS, FUS(16R). Both mutants strongly reduced axonal complexity in vivo. We also observed an axon looping defect for FUS(P525L) in the target area, which presumably arises due to errors in stop cue signaling. To assess whether the loss of axon complexity also had a cue-independent component, we assessed axonal cytoskeletal integrity in vitro. Using a novel combination of fluorescence and atomic force microscopy, we found that mutant FUS reduced actin density in the growth cone, altering its mechanical properties. Therefore, FUS mutants may induce defects during early axonal development.
Description
Keywords
Journal Title
Conference Name
Journal ISSN
1529-2401
Volume Title
Publisher
Publisher DOI
Sponsorship
Engineering and Physical Sciences Research Council (1946113)
Engineering and Physical Sciences Research Council (EP/L015889/1)
Engineering and Physical Sciences Research Council (EP/H018301/1)
Wellcome Trust (089703/Z/09/Z)
Wellcome Trust (215943/Z/19/Z)
Wellcome Trust (109145/Z/15/Z)
Medical Research Council (MR/K015850/1)
Medical Research Council (MR/K02292X/1)
European Research Council (772426)
Michael J. Fox Foundation (MJFF) (16238)
Alzheimer's Association (ZEN-18-529769)