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  A Dual Protein-mRNA Localization Screen Reveals Compartmentalized Translation and Widespread Co-translational RNA Targeting.

Chouaib, R., Safieddine, A., Pichon, X., Imbert, A., Kwon, O. S., Samacoits, A., et al. (2020). A Dual Protein-mRNA Localization Screen Reveals Compartmentalized Translation and Widespread Co-translational RNA Targeting. Developmental cell, 54(6), 773-791. doi:10.1016/j.devcel.2020.07.010.

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 Creators:
Chouaib, Racha, Author
Safieddine, Adham, Author
Pichon, Xavier, Author
Imbert, Arthur, Author
Kwon, Oh Sung, Author
Samacoits, Aubin, Author
Traboulsi, Abdel-Meneem, Author
Robert, Marie-Cécile, Author
Tsanov, Nikolay, Author
Coleno, Emeline, Author
Poser, Ina1, Author           
Zimmer, Christophe, Author
Hyman, Anthony1, Author           
Hir, Hervé Le, Author
Zibara, Kazem, Author
Peter, Matthias, Author
Mueller, Florian, Author
Walter, Thomas, Author
Bertrand, Edouard, Author
Affiliations:
1Max Planck Institute for Molecular Cell Biology and Genetics, Max Planck Society, ou_2340692              

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 Abstract: Local translation allows spatial control of gene expression. Here, we performed a dual protein-mRNA localization screen, using smFISH on 523 human cell lines expressing GFP-tagged genes. 32 mRNAs displayed specific cytoplasmic localizations with local translation at unexpected locations, including cytoplasmic protrusions, cell edges, endosomes, Golgi, the nuclear envelope, and centrosomes, the latter being cell-cycle-dependent. Automated classification of mRNA localization patterns revealed a high degree of intercellular heterogeneity. Surprisingly, mRNA localization frequently required ongoing translation, indicating widespread co-translational RNA targeting. Interestingly, while P-body accumulation was frequent (15 mRNAs), four mRNAs accumulated in foci that were distinct structures. These foci lacked the mature protein, but nascent polypeptide imaging showed that they were specialized translation factories. For β-catenin, foci formation was regulated by Wnt, relied on APC-dependent polysome aggregation, and led to nascent protein degradation. Thus, translation factories uniquely regulate nascent protein metabolism and create a fine granular compartmentalization of translation.

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 Dates: 2020-09-28
 Publication Status: Issued
 Pages: -
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 Table of Contents: -
 Rev. Type: -
 Identifiers: DOI: 10.1016/j.devcel.2020.07.010
Other: cbg-7735
PMID: 32783880
 Degree: -

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Title: Developmental cell
  Other : Dev Cell
Source Genre: Journal
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Pages: - Volume / Issue: 54 (6) Sequence Number: - Start / End Page: 773 - 791 Identifier: -