| Literature DB >> 33217318 |
Hagai Marmor-Kollet1, Aviad Siany1, Nancy Kedersha2, Naama Knafo3, Natalia Rivkin1, Yehuda M Danino1, Thomas G Moens4, Tsviya Olender1, Daoud Sheban5, Nir Cohen1, Tali Dadosh6, Yoseph Addadi7, Revital Ravid1, Chen Eitan1, Beata Toth Cohen1, Sarah Hofmann2, Claire L Riggs2, Vivek M Advani2, Adrian Higginbottom8, Johnathan Cooper-Knock8, Jacob H Hanna1, Yifat Merbl9, Ludo Van Den Bosch4, Paul Anderson2, Pavel Ivanov2, Tamar Geiger10, Eran Hornstein11.
Abstract
Stress granules (SGs) are cytoplasmic assemblies of proteins and non-translating mRNAs. Whereas much has been learned about SG formation, a major gap remains in understanding the compositional changes SGs undergo during normal disassembly and under disease conditions. Here, we address this gap by proteomic dissection of the SG temporal disassembly sequence using multi-bait APEX proximity proteomics. We discover 109 novel SG proteins and characterize distinct SG substructures. We reveal dozens of disassembly-engaged proteins (DEPs), some of which play functional roles in SG disassembly, including small ubiquitin-like modifier (SUMO) conjugating enzymes. We further demonstrate that SUMOylation regulates SG disassembly and SG formation. Parallel proteomics with amyotrophic lateral sclerosis (ALS)-associated C9ORF72 dipeptides uncovered attenuated DEP recruitment during SG disassembly and impaired SUMOylation. Accordingly, SUMO activity ameliorated C9ORF72-ALS-related neurodegeneration in Drosophila. By dissecting the SG spatiotemporal proteomic landscape, we provide an in-depth resource for future work on SG function and reveal basic and disease-relevant mechanisms of SG disassembly.Entities:
Keywords: ALS; APEX; RNA binding proteins; amyotrophic lateral sclerosis; condensates; membraneless organelles; neurodegeneration; phase separation; stress granules; sumoylation
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Year: 2020 PMID: 33217318 DOI: 10.1016/j.molcel.2020.10.032
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970