The mRNA encoding the JUND tumor suppressor detains nuclear RNA-binding proteins to assemble polysomes that are unaffected by mTOR

Singh, Gatikrushna; Fritz, Sarah E.; Seufzer, Bradley J.; Boris‐Lawrie, Kathleen

doi:10.1074/jbc.ra119.012005

Cited by 15 publications

(25 citation statements)

References 57 publications

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“…Indeed, the polysomes of HIV-1 Rev/RRE-dependent RNAs have failed to enrich eIF4E and instead engage a CBP80 mRNP ( 27 ). Recently, NCBP3/CBP80 heterodimer has been shown to assemble JUND polysomes for cap-dependent translation without eIF4E ( 21 ). To test whether TMG-capped HIV-1 mRNPs enriched eIF4E or NCBP3, the messenger ribonucleoproteins (mRNPs) were collected from HIV-infected, primary CD4 + T lymphocytes and subjected to RT-qPCR, as summarized in Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Torin-1 is a selective catalytic site mTOR inhibitor that up-regulates hypophosphorylated 4E-BP1 ( 21 , 28 , 29 ). Lymphocytes were infected with HIV NL4-3 for 6 h (multiplicity of infection [MOI] = 1), washed, and continuously cultured with or without Torin-1.…”

Section: Resultsmentioning

confidence: 99%

“…The junD mRNA maintains translation during mTOR inhibition yet fails conventional tests for cap-independent translation by an internal ribosome entry mechanism ( 20 ). Recently, the heterodimeric CBP80/NCBP3 has been shown to assemble JUND polysomes ( 21 ). The CBP80-NCBP3 heterodimer had been characterized in conditions of metabolic stress and viral infection and has been assigned roles in antiviral defense and RNA export that remain under investigation ( 22 , 23 ).…”

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confidence: 99%

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HIV-1 hypermethylated guanosine cap licenses specialized translation unaffected by mTOR

Singh

Seufzer

Song

et al. 2021

Proc. Natl. Acad. Sci. U.S.A.

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Appended to the 5′ end of nascent RNA polymerase II transcripts is 7-methyl guanosine (m7G-cap) that engages nuclear cap-binding complex (CBC) to facilitate messenger RNA (mRNA) maturation. Mature mRNAs exchange CBC for eIF4E, the rate-limiting translation factor that is controlled through mTOR. Experiments in immune cells have now documented HIV-1 incompletely processed transcripts exhibited hypermethylated m7G-cap and that the down-regulation of the trimethylguanosine synthetase-1–reduced HIV-1 infectivity and virion protein synthesis by several orders of magnitude. HIV-1 cap hypermethylation required nuclear RNA helicase A (RHA)/DHX9 interaction with the shape of the 5′ untranslated region (UTR) primer binding site (PBS) segment. Down-regulation of RHA or the anomalous shape of the PBS segment abrogated hypermethylated caps and derepressed eIF4E binding for virion protein translation during global down-regulation of host translation. mTOR inhibition was detrimental to HIV-1 proliferation and attenuated Tat, Rev, and Nef synthesis. This study identified mutually exclusive translation pathways and the calibration of virion structural/accessory protein synthesis with de novo synthesis of the viral regulatory proteins. The hypermethylation of select, viral mRNA resulted in CBC exchange to heterodimeric CBP80/NCBP3 that expanded the functional capacity of HIV-1 in immune cells.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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confidence: 99%

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HIV-1 hypermethylated guanosine cap licenses specialized translation unaffected by mTOR

Singh

Seufzer

Song

et al. 2021

Proc. Natl. Acad. Sci. U.S.A.

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“…The HIV late RNAs have been shown to specifically retain nuclear cap-binding complex (CBC) in polysomes and virions, instead of exchanging to eIF4E [ 56 ]. Recently, polysomal CBC RNPs were shown to activate eIF4E-independent translation of stress response proteins, overcoming AP-1 protein translation attenuation by mTOR inhibition [ 57 ]. Structural malleability near the HIV 5′-Cap may be beneficial to regulate cap-exchange and antagonize antiviral mTOR inhibition.…”

Section: Discussionmentioning

confidence: 99%

A New Approach to 3D Modeling of Inhomogeneous Populations of Viral Regulatory RNA

Osmer

Singh

Boris‐Lawrie

2020

Viruses

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Tertiary structure (3D) is the physical context of RNA regulatory activity. Retroviruses are RNA viruses that replicate through the proviral DNA intermediate transcribed by hosts. Proviral transcripts form inhomogeneous populations due to variable structural ensembles of overlapping regulatory RNA motifs in the 5′-untranslated region (UTR), which drive RNAs to be spliced or translated, and/or dimerized and packaged into virions. Genetic studies and structural techniques have provided fundamental input constraints to begin predicting HIV 3D conformations in silico. Using SimRNA and sets of experimentally-determined input constraints of HIVNL4-3 trans-activation responsive sequence (TAR) and pairings of unique-5′ (U5) with dimerization (DIS) or AUG motifs, we calculated a series of 3D models that differ in proximity of 5′-Cap and the junction of TAR and PolyA helices; configuration of primer binding site (PBS)-segment; and two host cofactors binding sites. Input constraints on U5-AUG pairings were most compatible with intramolecular folding of 5′-UTR motifs in energetic minima. Introducing theoretical constraints predicted metastable PolyA region drives orientation of 5′-Cap with TAR, U5 and PBS-segment helices. SimRNA and the workflow developed herein provides viable options to predict 3D conformations of inhomogeneous populations of large RNAs that have been intractable to conventional ensemble methods.

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“…The deposition of nuclear factors to pre-mRNA is necessary for nucleo-cytoplasmic transport and subsequent commitment to decay, storage or efficient translation to protein (Le Hir et al, 2001;Singh et al, 2020). circRNAs that are derived from introns (circular intronic RNAs, ciRNAs), remain in the nucleus and may regulate transcription of parental genes (Zhang et al, 2013;Zang et al, 2020) (Figure 1).…”

Section: A Prelude To Discovering a Full Repertoire Of Functionalitiementioning

confidence: 99%

Circular RNAs Are Regulators of Diverse Animal Transcriptomes: One Health Perspective

Zucko

Boris‐Lawrie

2020

Front. Genet.

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Derived from linear (parental) precursor mRNA, circRNA are recycled exons and introns whose ends are ligated. By titrating microRNAs and RNA binding proteins, circRNA interconnect networks of competing endogenous RNAs. Without altering chromosomal DNA, circRNA regulates skeletal muscle development and proliferation, lactation, ovulation, brain development, and responses to infections and metabolic stress. This review integrates emerging knowledge of circRNA activity coming from genome-wide characterizations in many clades of animals. circRNA research addresses one of the main pillars of the One Health vision-to improve the health and productivity of food animals and generate translational knowledge in animal species.

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The mRNA encoding the JUND tumor suppressor detains nuclear RNA-binding proteins to assemble polysomes that are unaffected by mTOR

Cited by 15 publications

References 57 publications

HIV-1 hypermethylated guanosine cap licenses specialized translation unaffected by mTOR

HIV-1 hypermethylated guanosine cap licenses specialized translation unaffected by mTOR

A New Approach to 3D Modeling of Inhomogeneous Populations of Viral Regulatory RNA

Circular RNAs Are Regulators of Diverse Animal Transcriptomes: One Health Perspective

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