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logo citeas Liu, C., Mentzelopoulou, A., Muhammad, A., Volkov, A., Weijers, D., Gutierrez‐Beltran, E., & Moschou, P. N. (2023, February 6). An actin remodeling role for Arabidopsis processing bodies revealed by their proximity interactome. The EMBO Journal. Springer Science and Business Media LLC. http://doi.org/10.15252/embj.2022111885
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Título

An actin remodeling role for Arabidopsis processing bodies revealed by their proximity interactome

AutorLiu, Chen; Mentzelopoulou, Andriani; Muhammad, Amna; Volkov, Andriy; Weijers, Dolf; Gutierrez-Beltran, Emilio ; Moschou, Panagiotis N
FinanciadoresEuropean Commission
Carl Trygger Foundation
Swedish Research Council for Sustainable Development
Helge Ax:son Johnsons Stiftelse
Ministerio de Ciencia, Innovación y Universidades (España)
Agencia Estatal de Investigación (España)
Palabras claveARP2-ARP3
LLPS
SCAR-WAVE
Condensates
Plasma membrane domains
Fecha de publicación2-may-2023
EditorEMBO Press
Springer
CitaciónThe EMBO Journal 42 (9):e111885 (2023)
ResumenCellular condensates can comprise membrane-less ribonucleoprotein assemblies with liquid-like properties. These cellular condensates influence various biological outcomes, but their liquidity hampers their isolation and characterization. Here, we investigated the composition of the condensates known as processing bodies (PBs) in the model plant Arabidopsis thaliana through a proximity-biotinylation proteomics approach. Using in situ protein-protein interaction approaches, genetics and high-resolution dynamic imaging, we show that processing bodies comprise networks that interface with membranes. Surprisingly, the conserved component of PBs, DECAPPING PROTEIN 1 (DCP1), can localize to unique plasma membrane subdomains including cell edges and vertices. We characterized these plasma membrane interfaces and discovered a developmental module that can control cell shape. This module is regulated by DCP1, independently from its role in decapping, and the actin-nucleating SCAR-WAVE complex, whereby the DCP1-SCAR-WAVE interaction confines and enhances actin nucleation. This study reveals an unexpected function for a conserved condensate at unique membrane interfaces.
Versión del editorhttps://doi.org/10.15252/embj.2022111885
URIhttp://hdl.handle.net/10261/354651
DOI10.15252/embj.2022111885
ISSN0261-4189
E-ISSN1460-2075
Licencia de usohttps://creativecommons.org/licenses/by/3.0/
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