Journal Article DZNE-2020-04773

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Monomethylated and unmethylated FUS exhibit increased binding to Transportin and distinguish FTLD-FUS from ALS-FUS.

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2016
Springer Heidelberg

Acta neuropathologica 131(4), 587-604 () [10.1007/s00401-016-1544-2]

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Abstract: Deposition of the nuclear DNA/RNA-binding protein Fused in sarcoma (FUS) in cytosolic inclusions is a common hallmark of some cases of frontotemporal lobar degeneration (FTLD-FUS) and amyotrophic lateral sclerosis (ALS-FUS). Whether both diseases also share common pathological mechanisms is currently unclear. Based on our previous finding that FUS deposits are hypomethylated in FTLD-FUS but not in ALS-FUS, we have now investigated whether genetic or pharmacological inactivation of Protein arginine methyltransferase 1 (PRMT1) activity results in unmethylated FUS or in alternatively methylated forms of FUS. To do so, we generated FUS-specific monoclonal antibodies that specifically recognize unmethylated arginine (UMA), monomethylated arginine (MMA) or asymmetrically dimethylated arginine (ADMA). Loss of PRMT1 indeed not only results in an increase of UMA FUS and a decrease of ADMA FUS, but also in a significant increase of MMA FUS. Compared to ADMA FUS, UMA and MMA FUS exhibit much higher binding affinities to Transportin-1, the nuclear import receptor of FUS, as measured by pull-down assays and isothermal titration calorimetry. Moreover, we show that MMA FUS occurs exclusively in FTLD-FUS, but not in ALS-FUS. Our findings therefore provide additional evidence that FTLD-FUS and ALS-FUS are caused by distinct disease mechanisms although both share FUS deposits as a common denominator.

Keyword(s): Amyotrophic Lateral Sclerosis: genetics (MeSH) ; Amyotrophic Lateral Sclerosis: metabolism (MeSH) ; Animals (MeSH) ; Antibodies: pharmacology (MeSH) ; Arginine: metabolism (MeSH) ; Cells, Cultured (MeSH) ; Cerebral Cortex: cytology (MeSH) ; Embryo, Mammalian (MeSH) ; Embryonic Stem Cells (MeSH) ; Enzyme Inhibitors: pharmacology (MeSH) ; Female (MeSH) ; Frontotemporal Lobar Degeneration: genetics (MeSH) ; Frontotemporal Lobar Degeneration: metabolism (MeSH) ; Humans (MeSH) ; Inclusion Bodies: drug effects (MeSH) ; Inclusion Bodies: metabolism (MeSH) ; Male (MeSH) ; Methylation (MeSH) ; Mice (MeSH) ; Mice, Inbred C57BL (MeSH) ; Mice, Knockout (MeSH) ; Neurons: drug effects (MeSH) ; Neurons: metabolism (MeSH) ; Protein Binding: drug effects (MeSH) ; Protein Binding: genetics (MeSH) ; Protein-Arginine N-Methyltransferases: genetics (MeSH) ; Protein-Arginine N-Methyltransferases: metabolism (MeSH) ; RNA-Binding Protein FUS: immunology (MeSH) ; RNA-Binding Protein FUS: metabolism (MeSH) ; Rats (MeSH) ; beta Karyopherins: immunology (MeSH) ; beta Karyopherins: metabolism (MeSH) ; Antibodies ; Enzyme Inhibitors ; RNA-Binding Protein FUS ; TNPO1 protein, human ; beta Karyopherins ; Arginine ; Protein-Arginine N-Methyltransferases

Classification:

Contributing Institute(s):
  1. Molecular Neuropathology of Neurodegenerative Diseases (AG Neumann)
  2. Clinical Neurodegeneration (AG Levin)
  3. Cell Biology of Neurodegeneration (AG Edbauer)
  4. Molecular Neurodegeneration (AG Haass)
Research Program(s):
  1. 344 - Clinical and Health Care Research (POF3-344) (POF3-344)
  2. 342 - Disease Mechanisms and Model Systems (POF3-342) (POF3-342)

Appears in the scientific report 2016
Database coverage:
Medline ; BIOSIS Previews ; Clarivate Analytics Master Journal List ; Current Contents - Life Sciences ; Ebsco Academic Search ; IF >= 15 ; JCR ; NCBI Molecular Biology Database ; NationallizenzNationallizenz ; SCOPUS ; Science Citation Index ; Science Citation Index Expanded ; Web of Science Core Collection
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Document types > Articles > Journal Article
Institute Collections > TÜ DZNE > TÜ DZNE-AG Neumann
Institute Collections > M DZNE > M DZNE-AG Edbauer
Institute Collections > M DZNE > M DZNE-AG Haass
Institute Collections > M DZNE > M DZNE-AG Levin
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 Record created 2020-02-18, last modified 2024-06-13


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