No-go decay: a quality control mechanism for RNA in translation.

Harigaya Y; Parker R

doi:10.1002/wrna.17

Abstract

Eukaryotic cells have evolved multiple quality control mechanisms that recognize and eliminate defective mRNA during the process of translation. One mechanism, referred to as No-go decay (NGD), targets mRNAs with elongation stalls for degradation initiated by endonucleolytic cleavage in the vicinity of the stalled ribosome. NGD is promoted by the evolutionarily conserved Dom34 and Hbs1 proteins, which are related to the translation termination factors eRF1 and eRF3, respectively. NGD is likely to occur by Dom34/Hbs1 interacting with the A site in the ribosome leading to release of the peptide or peptidyl-tRNA. The process of NGD and/or the function of Dom34/Hbs1 appear to be important in several different biological contexts.

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No-go decay: a quality control mechanism for RNA in translation.

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Abstract

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References

Quality control of eukaryotic mRNA: safeguarding cells from abnormal mRNA function.

RNA quality control in eukaryotes.

The many pathways of RNA degradation.

Regulation of translation initiation in eukaryotes: mechanisms and biological targets.

The mechanism of eukaryotic translation initiation and principles of its regulation.

Structural studies of elongation and release factors.

The termination of translation.

Fidelity at the molecular level: lessons from protein synthesis.

Hypusine-containing protein eIF5A promotes translation elongation.

In vitro reconstitution of eukaryotic translation reveals cooperativity between release factors eRF1 and eRF3.

Citations & impact

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Citations of article over time

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Smart citations by scite.ai
Explore citation contexts and check if this article has been supported or disputed.
https://scite.ai/reports/10.1002/wrna.17

Article citations

Picornavirus Evolution: Genomes Encoding Multiple 2A<sup>NPGP</sup> Sequences-Biomedical and Biotechnological Utility.

Ribosome stalling during c-myc translation presents actionable cancer cell vulnerability.

Stalled translation by mitochondrial stress upregulates a CNOT4-ZNF598 ribosomal quality control pathway important for tissue homeostasis.

Functional Characterization of Two Novel Intron 4 SERPING1 Gene Splice Site Pathogenic Variants in Families with Hereditary Angioedema.

Gene dosage compensation: Origins, criteria to identify compensated genes, and mechanisms including sensor loops as an emerging systems-level property in cancer.

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No-go decay: a quality control mechanism for RNA in translation.

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