ABCE1 is essential for S phase progression in human cells

Toompuu, Marina; Kärblane, Kairi; Pata, Pille; Truve, Erkki; Sarmiento, Cecilia

doi:10.1080/15384101.2016.1160972

Cited by 10 publications

(10 citation statements)

References 104 publications

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“…Since NMD is dependent on active translation ( 78 , 79 ), we next examined whether ABCE1 depletion might inhibit NMD indirectly by causing a global translation inhibition. Notably, a previous study has reported that ABCE1 KD in human cells reduces the general translation level ( 80 ). To assess the overall translation activity in control and ABCE1 KD cells, we pulse-chased HeLa cells with puromycin and detected puromycylated nascent polypeptide chains using an antibody against puromycin (Figure 3A ).…”

Section: Resultsmentioning

confidence: 99%

Readthrough of stop codons under limiting ABCE1 concentration involves frameshifting and inhibits nonsense-mediated mRNA decay

Annibaldis

Domanski

Dreos

et al. 2020

Nucleic Acids Research

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To gain insight into the mechanistic link between translation termination and nonsense-mediated mRNA decay (NMD), we depleted the ribosome recycling factor ABCE1 in human cells, resulting in an upregulation of NMD-sensitive mRNAs. Suppression of NMD on these mRNAs occurs prior to their SMG6-mediated endonucleolytic cleavage. ABCE1 depletion caused ribosome stalling at termination codons (TCs) and increased ribosome occupancy in 3′ UTRs, implying enhanced TC readthrough. ABCE1 knockdown indeed increased the rate of readthrough and continuation of translation in different reading frames, providing a possible explanation for the observed NMD inhibition, since enhanced readthrough displaces NMD activating proteins from the 3′ UTR. Our results indicate that stalling at TCs triggers ribosome collisions and activates ribosome quality control. Collectively, we show that improper translation termination can lead to readthrough of the TC, presumably due to ribosome collisions pushing the stalled ribosomes into the 3′ UTR, where it can resume translation in-frame as well as out-of-frame.

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Section: Resultsmentioning

confidence: 99%

Readthrough of stop codons under limiting ABCE1 concentration involves frameshifting and inhibits nonsense-mediated mRNA decay

Annibaldis

Domanski

Dreos

et al. 2020

Nucleic Acids Research

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“…These data support a requirement for Fe-S cluster biogenesis and ABCE1 in NMD. It has been reported that depletion of ABCE1 globally reduces translation (Toompuu et al, 2016). Because of the dependency of NMD on active translation, this could potentially account for impaired decay of nonsense transcripts in ABCE1-deficient cells.…”

Section: Deficiency Of Fe-s Clustermentioning

confidence: 99%

Ribosome Recycling by ABCE1 Links Lysosomal Function and Iron Homeostasis to 3ʹ UTR-Directed Regulation and Nonsense-Mediated Decay

2020

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“…Since NMD is dependent on active translation (Carter et al, 1995;Thermann et al, 1998), we next examined whether ABCE1 depletion might inhibit NMD indirectly by causing a global translation inhibition. Notably, a previous study has reported that ABCE1 KD in human cells reduces the general translation level (Toompuu et al, 2016). To assess the overall translation activity in control and ABCE1 KD cells, we pulse-chased HeLa cells with puromycin and detected puromycylated nascent polypeptide chains using an antibody against puromycin (Fig.…”

Section: Nmd Sensitive Mrnas Are Strongly Associated With Polysomes Imentioning

confidence: 99%

Ribosome recycling factor ABCE1 depletion inhibits nonsense-mediated mRNA decay by promoting stop codon readthrough

Annibaldis

Dreos

Domanski

et al. 2019

Preprint

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Highlights• ABCE1 knockdown suppresses NMD of many NMD-sensitive mRNAs• The observed NMD inhibition occurs at a stage prior to SMG6-mediated cleavage of the mRNA • ABCE1 depletion enhances ribosome occupancy at stop codons and in the 3' UTR• ABCE1 depletion enhances readthrough of the stop codon• Enhanced readthrough inhibits NMD, presumably by clearing the 3' UTR of NMD factors SUMMARY Nonsense-mediated mRNA decay (NMD) is an essential post-transcriptional surveillance pathway in vertebrates that appears to be mechanistically linked with translation termination. To gain more insight into this connection, we interfered with translation termination by depleting human cells of the ribosome recycling factor ABCE1, which resulted in an upregulation of many but not all endogenous NMD-sensitive mRNAs. Notably, the suppression of NMD on these mRNAs occurs at a step prior to their SMG6-mediated endonucleolytic cleavage. Ribosome profiling revealed that ABCE1 depletion results in ribosome stalling at stop codons and increased ribosome occupancy in 3' UTRs, indicative of enhanced stop codon readthrough or re-initiation. Using reporter genes, we further demonstrate that the absence of ABCE1 indeed increases the rate of readthrough, which would explain the observed NMD inhibition, since enhanced readthrough has been previously shown to render NMD-sensitive transcripts resistant to NMD by displacing NMD triggering factors like UPF1 and exon junction complexes (EJCs) from the 3' UTR. Collectively, our results show that improper ribosome disassembly interferes with proper NMD activation.indicates that NMD ensues when a ribosome stalls at a termination codon (TC) for prolonged time because of a failure to properly or fast enough terminate translation (Amrani et al., 2004;Peixeiro et al., 2011). On mRNA with problems in translation termination, the so-called SURF complex (composed of SMG1, UPF1 and the release factors eRF1 and eRF3) was proposed to assemble at the TC (Ivanov et al., 2008;Kashima et al., 2006;Singh et al., 2008). SMG1-mediated phosphorylation of UPF1, a core factor of NMD, appears to be a key event in activating NMD, because hyper-phosphorylated UPF1 subsequently serves as a binding platform for the heterodimer SMG5/SMG7 and for the endonuclease SMG6, allowing for two different decay routes (Muhlemann and Lykke-Andersen, 2010). A third decay pathway operating via SMG5 and PNRC2 has also been proposed (Cho et al., 2013) but remains controversial (Loh et al., 2013;Nicholson et al., 2018). Moreover, a recent study challenged the SURF complex-based NMD activation model by showing that UPF3B rather than UPF1 interacts with the release factors (Neu-Yilik et al.

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ABCE1 is essential for S phase progression in human cells

Cited by 10 publications

References 104 publications

Readthrough of stop codons under limiting ABCE1 concentration involves frameshifting and inhibits nonsense-mediated mRNA decay

Readthrough of stop codons under limiting ABCE1 concentration involves frameshifting and inhibits nonsense-mediated mRNA decay

Ribosome Recycling by ABCE1 Links Lysosomal Function and Iron Homeostasis to 3ʹ UTR-Directed Regulation and Nonsense-Mediated Decay

Ribosome recycling factor ABCE1 depletion inhibits nonsense-mediated mRNA decay by promoting stop codon readthrough

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