Loss of mitochondrial ClpP, Lonp1, and Tfam triggers transcriptional induction of Rnf213, a susceptibility factor for moyamoya disease

  1. Key, Jana
  2. Maletzko, Antonia
  3. Kohli, Aneesha
  4. Gispert, Suzana
  5. Torres-Odio, Sylvia
  6. Wittig, Ilka
  7. Heidler, Juliana
  8. Bárcena, Clea
  9. López-Otín, Carlos
  10. Lei, Yuanjiu
  11. West, A. Phillip
  12. Münch, Christian
  13. Auburger, Georg

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1000 Titel
  • Loss of mitochondrial ClpP, Lonp1, and Tfam triggers transcriptional induction of Rnf213, a susceptibility factor for moyamoya disease
1000 Autor/in
  1. Key, Jana |
  2. Maletzko, Antonia |
  3. Kohli, Aneesha |
  4. Gispert, Suzana |
  5. Torres-Odio, Sylvia |
  6. Wittig, Ilka |
  7. Heidler, Juliana |
  8. Bárcena, Clea |
  9. López-Otín, Carlos |
  10. Lei, Yuanjiu |
  11. West, A. Phillip |
  12. Münch, Christian |
  13. Auburger, Georg |
1000 Erscheinungsjahr 2020
1000 Publikationstyp
  1. Artikel |
1000 Online veröffentlicht
  • 2020-04-28
1000 Erschienen in
1000 Quellenangabe
  • 21(3):187-203
1000 Copyrightjahr
  • 2020
1000 Lizenz
1000 Verlagsversion
  • https://doi.org/10.1007/s10048-020-00609-2 |
  • https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7283203/ |
1000 Publikationsstatus
1000 Sprache der Publikation
1000 Abstract/Summary
  • Human RNF213, which encodes the protein mysterin, is a known susceptibility gene for moyamoya disease (MMD), a cerebrovascular condition with occlusive lesions and compensatory angiogenesis. Mysterin mutations, together with exposure to environmental trigger factors, lead to an elevated stroke risk since childhood. Mysterin is induced during cell stress, to function as cytosolic AAA+ ATPase and ubiquitylation enzyme. Little knowledge exists, in which context mysterin is needed. Here, we found that genetic ablation of several mitochondrial matrix factors, such as the peptidase ClpP, the transcription factor Tfam, as well as the peptidase and AAA+ ATPase Lonp1, potently induces Rnf213 transcript expression in various organs, in parallel with other components of the innate immune system. Mostly in mouse fibroblasts and human endothelial cells, the Rnf213 levels showed prominent upregulation upon Poly(I:C)-triggered TLR3-mediated responses to dsRNA toxicity, as well as upon interferon gamma treatment. Only partial suppression of Rnf213 induction was achieved by C16 as an antagonist of PKR (dsRNA-dependent protein kinase). Since dysfunctional mitochondria were recently reported to release immune-stimulatory dsRNA into the cytosol, our results suggest that mysterin becomes relevant when mitochondrial dysfunction or infections have triggered RNA-dependent inflammation. Thus, MMD has similarities with vasculopathies that involve altered nucleotide processing, such as Aicardi-Goutières syndrome or systemic lupus erythematosus. Furthermore, in MMD, the low penetrance of RNF213 mutations might be modified by dysfunctions in mitochondria or the TLR3 pathway.
1000 Sacherschließung
lokal Cell Line, Tumor [MeSH]
lokal Transcription Factors/genetics [MeSH]
lokal Inflammation [MeSH]
lokal Interferon-gamma/metabolism [MeSH]
lokal Macrophages/metabolism [MeSH]
lokal Ubiquitin-Protein Ligases/genetics [MeSH]
lokal Poly I-C [MeSH]
lokal DNA-Binding Proteins/genetics [MeSH]
lokal Cytosol/metabolism [MeSH]
lokal Original Article
lokal Adenosine Triphosphatases/genetics [MeSH]
lokal Autoimmune vasculopathy
lokal Immune System [MeSH]
lokal Innate immunity
lokal Mitochondrial Proteins/genetics [MeSH]
lokal Human Umbilical Vein Endothelial Cells [MeSH]
lokal Ubiquitin ligase
lokal ATP-Dependent Proteases/genetics [MeSH]
lokal Moyamoya Disease/genetics [MeSH]
lokal Mass Spectrometry [MeSH]
lokal Proteome [MeSH]
lokal Fibroblasts/metabolism [MeSH]
lokal Mutation [MeSH]
lokal Mitochondria/metabolism [MeSH]
lokal Stroke genetics
lokal Humans [MeSH]
lokal Lipopolysaccharides/metabolism [MeSH]
lokal AAA disaggregase
lokal Mitochondrial dysfunction
lokal Animals [MeSH]
lokal Endopeptidase Clp/genetics [MeSH]
lokal RNA/metabolism [MeSH]
lokal Mice [MeSH]
lokal Protein Folding [MeSH]
lokal Perrault syndrome
lokal Transcriptome [MeSH]
lokal Gene Expression Profiling [MeSH]
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