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  Mechanisms of readthrough mitigation reveal principles of GCN1-mediated translational quality control

Müller, M. B. D., Kasturi, P., Jayaraj, G. G., & Hartl, F. U. (2023). Mechanisms of readthrough mitigation reveal principles of GCN1-mediated translational quality control. Cell, 186(15), 3227-3244. doi:10.1016/j.cell.2023.05.035.

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 Creators:
Müller, Martin B. D.1, Author           
Kasturi, Prasad1, Author           
Jayaraj, Gopal G.1, Author           
Hartl, F. Ulrich1, Author           
Affiliations:
1Hartl, Franz-Ulrich / Cellular Biochemistry, Max Planck Institute of Biochemistry, Max Planck Society, ou_1565152              

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Free keywords: MESSENGER-RNA TRANSLATION; STOP CODON; CAENORHABDITIS-ELEGANS; MEMBRANE-PROTEINS; DEGRADATION; AGGREGATION; PROTEOSTASIS; TERMINATION; SURVEILLANCE; RECOGNITIONBiochemistry & Molecular Biology; Cell Biology;
 Abstract: Readthrough into the 3' untranslated region (3' UTR) of the mRNA results in the production of aberrant proteins. Metazoans efficiently clear readthrough proteins, but the underlying mechanisms remain unknown. Here, we show in Caenorhabditis elegans and mammalian cells that readthrough proteins are targeted by a coupled, two-level quality control pathway involving the BAG6 chaperone complex and the ribosome-collision-sensing protein GCN1. Readthrough proteins with hydrophobic C-terminal extensions (CTEs) are recognized by SGTABAG6 and ubiquitylated by RNF126 for proteasomal degradation. Additionally, cotranslational mRNA decay initiated by GCN1 and CCR4/NOT limits the accumulation of readthrough products. Unexpectedly, selective ribosome profiling uncovered a general role of GCN1 in regulating translation dynamics when ribosomes collide at nonoptimal codons, enriched in 3' UTRs, transmembrane proteins, and collagens. GCN1 dysfunction increasingly perturbs these protein classes during aging, resulting in mRNA and proteome imbalance. Our results define GCN1 as a key factor acting during translation in maintaining protein homeostasis.

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Language(s): eng - English
 Dates: 2023-06-192023-07-20
 Publication Status: Issued
 Pages: 39
 Publishing info: -
 Table of Contents: -
 Rev. Type: Peer
 Degree: -

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Project name : INSITUFOLD
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Funding organization : ERC

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Title: Cell
Source Genre: Journal
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Publ. Info: Cambridge, Mass. : Cell Press
Pages: - Volume / Issue: 186 (15) Sequence Number: - Start / End Page: 3227 - 3244 Identifier: ISSN: 0092-8674
CoNE: https://pure.mpg.de/cone/journals/resource/954925463183