Mutations in the 3′ untranslated region of FUS causing FUS overexpression are associated with amyotrophic lateral sclerosis

Sabatelli, Mario; Moncada, Alice; Conte, Amelia; Lattante, Serena; Marangi, Giuseppe; Luigetti, Marco; Lucchini, Matteo; Mirabella, Massimiliano; Romano, Ângela; Grande, Alessandra Del; Bisogni, Giulia; Doronzio, Paolo Niccolò; Rossini, Paolo Maria; Zollino, Marcella

doi:10.1093/hmg/ddt328

Cited by 97 publications

(104 citation statements)

References 27 publications

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“…The CAG-FUS WT and CAG-FUS R521G mouse models demonstrate that increased expression of FUS alone can cause cellular toxicity. This result is consistent with the recent finding that mutations in the 3′ UTR of FUS increase FUS expression levels and cause ALS (15). This result is also in agreement with end-stage pathological markers or outcomes in human patients.…”

Section: Differences and Commonalities In Fus Overexpression And Misssupporting

confidence: 93%

“…Besides missense mutations at the C terminus of FUS protein, overexpression of wild-type FUS caused by mutations in its 3′ UTR also has been linked to ALS (15), suggesting that overexpression of wild-type FUS is pathogenic under certain circumstances. Indeed, pathogenic effects of increased levels of wild-type proteins are common in other neurodegenerative disorders, as exemplified by increased gene dose or overexpression of wild-type TDP-43, α-synuclein, and amyloid β precursor protein (APP) in ALS/FTLD, Parkinson disease, and Alzheimer's disease (16)(17)(18).…”

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confidence: 99%

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Activity-dependent FUS dysregulation disrupts synaptic homeostasis

Sephton

Tang

Kulkarni

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

119

123

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The RNA-binding protein fused-in-sarcoma (FUS) has been associated with amyotrophic lateral sclerosis (ALS) and frontotemporal lobar degeneration (FTLD), two neurodegenerative disorders that share similar clinical and pathological features. Both missense mutations and overexpression of wild-type FUS protein can be pathogenic in human patients. To study the molecular and cellular basis by which FUS mutations and overexpression cause disease, we generated novel transgenic mice globally expressing low levels of human wild-type protein (FUS WT ) and a pathological mutation (FUS R521G A myotrophic lateral sclerosis (ALS) is characterized by the degeneration of upper and lower motor neurons, leading to muscle weakness, paralysis, and death within 3-5 y of onset. Interestingly, ∼10-15% of ALS patients have clinical features of frontotemporal lobar degeneration (FTLD), marked by a decline in decision-making, behavioral control, emotion, and language, and as many as half have mild-to-moderate cognitive or behavioral abnormalities (1). FTLD comprises a group of heterogeneous diseases characterized by progressive neurodegeneration of the frontal and temporal lobes and clinically by frontotemporal dementia (FTD) with or without motor neuron disease. There is no cure or effective therapy for those who suffer from ALS or FTLD, and the mechanisms by which these diseases occur are not well understood.The clinical, pathological, and genetic overlap between ALS and FTLD suggests that there are mechanisms shared by these diseases. The RNA-binding proteins fused in sarcoma (FUS) and transactive response DNA-binding protein-43 (TDP-43) are the major protein components of inclusions that are characteristic of ALS and FTLD-U (FTLD with ubiquitinated inclusions) (2). More than 50 genetic FUS mutations have been identified in these related neurodegenerative disorders (3). Similarly, more than 40 dominant mutations in the TDP-43 gene have been linked to ALS cases and, to a lesser extent, to FTLD (4). The identification of mutations in the FUS and TDP-43 genes has provided insights for uncovering the disease mechanisms for ALS and FTLD.FUS is a ubiquitously expressed RNA-binding protein that exists in dynamic ribonucleoprotein complexes involved in pre-mRNA splicing, mRNA stability, and mRNA transport. FUS is a member of the FET family of proteins that bind RNAs (5) and contains an RNA recognition motif, three arginine-glycine-glycine (RGG) boxes, and a zinc finger (ZnF) (6). RGG2-ZnF-RGG3 is the major RNA-binding domain, which has a preference for GUrich sequences (7,8). The N terminus of FUS contains a lowcomplexity sequence domain involved in RNA granule formation (9). Nucleocytoplasmic shuttling of FUS occurs by a nonclassical proline-tyrosine nuclear localization signal (PY-NLS) and a nuclear export signal (NES) (10). Methylation of the C-terminal RGG3 domain of FUS is necessary for transportin 1 interaction and nuclear localization (11).The majority of clinical ALS/FTLD-associated FUS mutations occur in its C-terminal PY-NLS seque...

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Section: Differences and Commonalities In Fus Overexpression And Misssupporting

confidence: 93%

mentioning

confidence: 99%

Activity-dependent FUS dysregulation disrupts synaptic homeostasis

Sephton

Tang

Kulkarni

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

119

123

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“…Nevertheless, the increase in FUS protein did not reach the levels observed with the entire deletion of the 3 0 -UTR (FUS-D3 0 -UTR), suggesting the presence of additional regulatory elements besides the MRE (miRNA recognition element) for miR-141/200a. This seems indeed to be the case since three other mutations, associated with severe ALS phenotypes and linked to high accumulation of protein, were also identified in this region 7 . However, according to TargetScan and PicTar analyses 12,13 , none of those mutations appear to affect conserved miRNA-binding sites.…”

Section: Resultsmentioning

confidence: 73%

“…Bioinformatics search 12,13 for miRNA-responsive elements in the FUS 3 0 -UTR indicated that among the identified 3 0 -UTR mutations 7 , two patients carried the G48A substitution (in one case of inherited type), which localizes to a predicted binding site for miR-141 and miR-200a. These two miRNAs share the same seed sequence and belong to the same miRNA family 14 The members of this family are of particular interest for human health and disease, because they have been shown to be downregulated during tumour progression and to act as key regulators of epithelial-to-mesenchymal transition 15 .…”

Section: Resultsmentioning

confidence: 99%

“…Most of these mutations alter the subcellular partitioning of the protein, which leads to a decrease of the nuclear content and an increase in the cytoplasm. Notably, recent sequencing of the 3 0 -untranslated region (3 0 -UTR) of FUS messenger RNA (mRNA) in 420 ALS patients, negative for mutations in the currently known ALS-associated genes, identified four mutations linked to severe outcomes that caused a strong increase in FUS accumulation 7 . The pathogenetic effects of wild-type (wt) FUS overexpression observed in these patients suggests that not only the nuclearcytoplasmic imbalance of the mutant protein, but also alteration of the physiological levels of the wt protein may contribute to ALS pathogenesis.…”

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confidence: 99%

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An ALS-associated mutation in the FUS 3′-UTR disrupts a microRNA–FUS regulatory circuitry

et al. 2014

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While the physiologic functions of the RNA-binding protein FUS still await thorough characterization, the pathonegetic role of FUS mutations in amyotrophic lateral sclerosis (ALS) is clearly established. Here we find that a human FUS mutation that leads to increased protein expression, and was identified in two ALS patients with severe outcome, maps to the seed sequence recognized by miR-141 and miR-200a in the 3 0 -UTR of FUS. We demonstrate that FUS and these microRNAs are linked by a feed-forward regulatory loop where FUS upregulates miR-141/200a, which in turn impact FUS protein synthesis. We also show that Zeb1, a target of miR-141/200a and transcriptional repressor of these two microRNAs, is part of the circuitry and reinforces it. Our results reveal a possible correlation between deregulation of this regulatory circuit and ALS pathogenesis, and open interesting perspectives in the treatment of these mutations through ad hoc-modified microRNAs.

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Genetic Basis of ALS

Ross

Rouleau

2021

Spectrums of Amyotrophic Lateral Sclerosis

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Mutations in the 3′ untranslated region of FUS causing FUS overexpression are associated with amyotrophic lateral sclerosis

Cited by 97 publications

References 27 publications

Activity-dependent FUS dysregulation disrupts synaptic homeostasis

Activity-dependent FUS dysregulation disrupts synaptic homeostasis

An ALS-associated mutation in the FUS 3′-UTR disrupts a microRNA–FUS regulatory circuitry

Genetic Basis of ALS

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