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Mislocalization of Nup62 Contributes to TDP-43 Proteinopathy in ALS/FTLD.

Niharika Nag, Timir Tripathi

ACS chemical neuroscience 2022 Sep 07


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  • FG (2)
  • glycoproteins (2)
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  • nuclear pore complex proteins (2)
  • nuclear pore protein p62 (1)
  • Nup62 (7)
  • pathogenesis (1)
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    The nucleocytoplasmic transport (NCT) is impaired in C9-ALS/FTLD, a common genetically caused form of ALS and FTLD. The NCT is regulated by proteins called FG-nucleoporins (FG-Nups), with domains enriched in phenylalanine-glycine repeats. However, the relationship between FG-Nups and TDP-43, an RBP found to be mislocalized in ALS/FTLD patients, has not been defined. A recent study found that a critical protein, FG-Nup62, is mislocalized both in vivo and in vitro in diseased states. The mislocalized Nup62 was colocalized with TDP-43 in cytoplasmic inclusions and promoted its liquid-to-solid transition. The work highlights the involvement of Nup62 in the pathogenesis of ALS/FTLD and the interaction between Nup62 and TDP-43.

    Citation

    Niharika Nag, Timir Tripathi. Mislocalization of Nup62 Contributes to TDP-43 Proteinopathy in ALS/FTLD. ACS chemical neuroscience. 2022 Sep 07;13(17):2544-2546

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    PMID: 36001801

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