| Literature DB >> 30989774 |
Urko Del Castillo1, Megan M Gnazzo2, Christopher G Sorensen Turpin3, Ken C Q Nguyen4, Emily Semaya4, Yuwan Lam5, Matthew A de Cruz5, Joshua N Bembenek3, David H Hall4, Blake Riggs5, Vladimir I Gelfand1, Ahna R Skop2.
Abstract
Ataxin-2, a conserved RNA-binding protein, is implicated in the late-onset neurodegenerative disease Spinocerebellar ataxia type-2 (SCA2). SCA2 is characterized by shrunken dendritic arbors and torpedo-like axons within the Purkinje neurons of the cerebellum. Torpedo-like axons have been described to contain displaced endoplasmic reticulum (ER) in the periphery of the cell; however, the role of Ataxin-2 in mediating ER function in SCA2 is unclear. We utilized the Caenorhabditis elegans and Drosophila homologs of Ataxin-2 (ATX-2 and DAtx2, respectively) to determine the role of Ataxin-2 in ER function and dynamics in embryos and neurons. Loss of ATX-2 and DAtx2 resulted in collapse of the ER in dividing embryonic cells and germline, and ultrastructure analysis revealed unique spherical stacks of ER in mature oocytes and fragmented and truncated ER tubules in the embryo. ATX-2 and DAtx2 reside in puncta adjacent to the ER in both C. elegans and Drosophila embryos. Lastly, depletion of DAtx2 in cultured Drosophila neurons recapitulated the shrunken dendritic arbor phenotype of SCA2. ER morphology and dynamics were severely disrupted in these neurons. Taken together, we provide evidence that Ataxin-2 plays an evolutionary conserved role in ER dynamics and morphology in C. elegans and Drosophila embryos during development and in fly neurons, suggesting a possible SCA2 disease mechanism.Entities:
Keywords: ATX-2; Ataxin-2; DAtx-2; RBPs; RNA; cytokinesis; endoplasmic reticulum; mitosis; neurons
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Year: 2019 PMID: 30989774 PMCID: PMC6553494 DOI: 10.1111/tra.12647
Source DB: PubMed Journal: Traffic ISSN: 1398-9219 Impact factor: 6.215