2′-O-ribose methylation of cap2 in human: function and evolution in a horizontally mobile family

Werner, Maria Fernanda de Paula; Purta, Elżbieta; Kamińska, Katarzyna; Cymerman, Iwona A.; Campbell, David A.; Mittra, Bidyottam; Zamudio, Jesse R.; Sturm, Nancy R.; Jaworski, Jacek; Bujnicki, Janusz M.

doi:10.1093/nar/gkr038

Cited by 122 publications

(115 citation statements)

References 55 publications

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“…The 2′- O -methylation of riboses near the 5′ ends of eukaryotic mRNAs serve as additional signals to distinguish normal uncapped cellular pre-mRNAs from viral RNAs (Daffis et al, 2010). Interestingly, the evolution of the eukaryotic cap methylation machinery appears to have involved horizontal gene transfer between eukaryotes and viruses, supporting the possibility of conflict between host and viruses with respect to these sugar modifications of mRNA (Werner et al, 2011). …”

Section: Antiviral Identification Cards For Messenger Rnamentioning

confidence: 99%

The Frustrated Gene: Origins of Eukaryotic Gene Expression

Madhani

2013

Cell

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Section: Antiviral Identification Cards For Messenger Rnamentioning

confidence: 99%

The Frustrated Gene: Origins of Eukaryotic Gene Expression

Madhani

2013

Cell

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“…In higher eukaryotes, additional methylation of mRNA occurs at the 2 ′ -O position of the first ribose sugar (m 7 GpppNm, cap 1 structure) via a nuclear 2 ′ -O methyltransferase enzyme. Because some IFIT family members (e.g., mouse Ifit1) directly recognize cap 0 RNA, host 2 ′ -O methylation serves to distinguish self and non-self RNA (Daffis et al, 2010; Werner et al, 2011; Zust et al, 2011). …”

Section: Introductionmentioning

confidence: 99%

Human IFIT3 Modulates IFIT1 RNA Binding Specificity and Protein Stability

et al. 2018

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SUMMARY Interferon-induced proteins with tetratricopeptide repeats (IFIT) inhibit infection of many viruses by recognizing their RNA, but the mechanisms regulating their remain unclear. We report a crystal structure of cap 0 (m7GpppN)-RNA-bound to human IFIT1 in complex with the C-terminal domain of human IFIT3. Structural, biochemical, and genetic studies suggest that IFIT3 binding to IFIT1 has dual regulatory functions: (a) extending the half-life of IFIT1, which increases its steady-state levels in cells and (b) allosterically regulating the IFIT1 RNA-binding channel, which enhances the specificity of recognition for cap 0 but not cap 1 (m7GpppNm) or 5′-ppp RNA. Mouse Ifit3 lacks this key C-terminal domain and does not bind mouse Ifit1. The IFIT3 interaction with IFIT1 was important for restricting infection of viruses lacking 2′-O methylation in their RNA cap structures. Our experiments establish differences in regulation of IFIT1 orthologs and define targets for modulating the activity of human IFIT proteins.

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“…5,6 Furthermore, in mammals the first 2 nucleotides are methylated on the O-2 position by CMTR1 and CMTR2. 7,8 O-2 methylation has roles in translation initiation and identifying transcripts as "self" in innate immunity. 4 …”

Section: Introductionmentioning

confidence: 99%

Regulation of mRNA capping in the cell cycle

Aregger

Cowling

2016

RNA Biology

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The mRNA cap structure, which is added to nascent RNA pol II transcripts, recruits the protein complexes required for pre-mRNA transcript processing, mRNA export and translation initiation. The enzymes which catalyze mRNA cap synthesis are regulated by cellular signaling pathways which impact on their expression, localization and activity. Here we discuss the recent observation that the mRNA cap methyltransferase, RNMT, is phosphorylated on Thr-77 by CDK1-cyclin B1, which regulates its activity and the proteins with which it interacts. RNMT Thr-77 phosphorylation provides a burst of mRNA cap methyltransferase activity during early G1 phase at a time when transcription is reactivated following completion of the cell cycle. This co-ordination of transcription and mRNA capping makes an important contribution to gene expression in the cell; preventing RNMT Thr-77 phosphorylation inhibits cell proliferation. Here we discuss these findings and how mRNA cap synthesis may be regulated in other scenarios.

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2′-O-ribose methylation of cap2 in human: function and evolution in a horizontally mobile family

Cited by 122 publications

References 55 publications

The Frustrated Gene: Origins of Eukaryotic Gene Expression

The Frustrated Gene: Origins of Eukaryotic Gene Expression

Human IFIT3 Modulates IFIT1 RNA Binding Specificity and Protein Stability

Regulation of mRNA capping in the cell cycle

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