Host Cell Interactome of HIV-1 Rev Includes RNA Helicases Involved in Multiple Facets of Virus Production

Naji, Souad; Ambrus, Géza; Cimermančič, Peter; Reyes, Jason R.; Johnson, Jeffrey R.; Filbrandt, Rebecca; Huber, Michael; Vesely, Paul; Krogan, Nevan J.; Yates, John R.; Saphire, Andrew C. S.; Gerace, Larry

doi:10.1074/mcp.m111.015313

Cited by 118 publications

(132 citation statements)

References 56 publications

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“…31 Our results support such a model in the control of vRNA encapsidation that involves subtle changes to the composition and trafficking of the HIV-1 RNP. hnRNP A2/B1 is a common component of several relevant HIV-1 complexes that have been recently characterized at the proteomics level 9,33,65 and these hnRNPs likely exert functions during the transit of HIV-1 complexes from the nucleus to and within the cytoplasm, perhaps acting in concert with Rev at multiple levels.…”

Section: Discussionmentioning

confidence: 99%

“…[6][7][8] Several host proteins have been shown to influence Rev's activity by direct interaction or by influencing the ribonucleoprotein (RNP) context of the RNA. [9][10][11][12] Rev also has effects on splicing regulation 13,14 as well as on downstream gene expression events at the translation level. [15][16][17] Efforts to understand Rev's functions during viral replication cycle have provided several key leads in the identification of potential therapeutic strategies and targets 18,19 and have provided critical information on the processes governing nuclear RNA export in general.…”

Section: Introductionmentioning

confidence: 99%

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Depletion of hnRNP A2/B1 overrides the nuclear retention of the HIV-1 genomic RNA

et al. 2013

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hnRNP A2 is a cellular protein that is important for nucleocytoplasmic and cytosolic trafficking of the hIV-1 genomic RNA. Both hnRNP A2's interaction with hIV-1 RNA and its expression levels influence the activities of Rev in mediating nucleocytoplasmic export of the hIV-1 genomic RNA. While the lack of Rev expression during hIV-1 gene expression results in nuclear retention of hIV-1 genomic RNA, we show here by fluorescence in situ hybridization and fractionation studies that the genomic RNA translocates to the cytoplasm when hnRNP A2/B1 are depleted from cells. Polyribosome analyses revealed that the genomic RNA was shunted into a cytoplasmic, dense polyribosomal fraction. This fraction contained several RNA-binding proteins involved in viral gene expression and RNA trafficking but did not contain the translation initiation factor, eIF4G1. Amino acid incorporation into nascent polypeptides in this fraction was also greatly reduced, demonstrating that this fraction contains mRNAs that are poorly translated. These results demonstrate that hnRNP A2/B1 expression plays roles in the nuclear retention of the hIV-1 genomic RNA in the absence of Rev and in the release of the genomic RNA from translationally inactive, cytoplasmic RNP complexes.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Depletion of hnRNP A2/B1 overrides the nuclear retention of the HIV-1 genomic RNA

et al. 2013

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“…We initially identified NonO interacting with PICs in HIV-1-infected CD4 + T cell lines, 9 and subsequent studies have also identified NonO to be an HIV-1 interactant. [10][11][12] However, the significance of these interactions and whether NonO plays a crucial role in HIV-1 infection have not been answered. We addressed these questions by investigating the effect of NonO KD on HIV-1 infection and characterized what stages of the replication cycle were affected.…”

Section: Discussionmentioning

confidence: 99%

“…11 Furthermore, NonO was identified in an analysis of the Rev interactome in HeLa cells, and the association between NonO and Rev was enhanced by the presence of the Rev response element. 12 These studies suggest that NonO may affect multiple steps of the HIV-1 lifecycle including integration. However, the role of NonO in HIV-1 infection has not been clearly characterized.…”

Section: Introductionmentioning

confidence: 99%

Non-POU Domain-Containing Octamer-Binding Protein Negatively Regulates HIV-1 Infection in CD4⁺T Cells

Gelais

Roger

2015

AIDS Research and Human Retroviruses

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HIV-1 interacts with numerous cellular proteins during viral replication. Identifying such host proteins and characterizing their roles in HIV-1 infection can deepen our understanding of the dynamic interplay between host and pathogen. We previously identified non-POU domain-containing octamer-binding protein (NonO or p54nrb) as one of host factors associated with catalytically active preintegration complexes (PIC) of HIV-1 in infected CD41 T cells. NonO is involved in nuclear processes including transcriptional regulation and RNA splicing. Although NonO has been identified as an HIV-1 interactant in several recent studies, its role in HIV-1 replication has not been characterized. We investigated the effect of NonO on the HIV-1 life cycle in CD4 1

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“…Extensive research has identified cellular proteins by direct and indirect interactions with Rev that facilitate transport of RRE-containing viral mRNA out of the nucleus [34,[42][43][44]. We had shown that a mutant Tat protein, we call Nullbasic, has an intriguing ability to inhibit Rev function resulting from its mislocalization from the nucleolus to the nucleoplasm and cytoplasm.…”

Section: Discussionmentioning

confidence: 99%

A HIV-1 Tat mutant protein disrupts HIV-1 Rev function by targeting the DEAD-box RNA helicase DDX1

et al. 2014

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Background: Previously we described a transdominant negative mutant of the HIV-1 Tat protein, termed Nullbasic, that downregulated the steady state levels of unspliced and singly spliced viral mRNA, an activity caused by inhibition of HIV-1 Rev activity. Nullbasic also altered the subcellular localizations of Rev and other cellular proteins, including CRM1, B23 and C23 in a Rev-dependent manner, suggesting that Nullbasic may disrupt Rev function and trafficking by intervening with an unidentified component of the Rev nucleocytoplasmic transport complex. Results: To seek a possible mechanism that could explain how Nullbasic inhibits Rev activity, we used a proteomics approach to identify host cellular proteins that interact with Nullbasic. Forty-six Nullbasic-binding proteins were identified by mass spectrometry including the DEAD-box RNA helicase, DDX1. To determine the effect of DDX1 on Nullbasic-mediated Rev activity, we performed cell-based immunoprecipitation assays, Rev reporter assays and bio-layer interferometry (BLI) assays. Interaction between DDX1 and Nullbasic was observed by co-immunoprecipitation of Nullbasic with endogenous DDX1 from cell lysates. BLI assays showed a direct interaction between Nullbasic and DDX1. Nullbasic affected DDX1 subcellular distribution in a Rev-independent manner. Interestingly overexpression of DDX1 in cells not only restored Rev-dependent mRNA export and gene expression in a Rev reporter assay but also partly reversed Nullbasic-induced Rev subcellular mislocalization. Moreover, HIV-1 wild type Tat co-immunoprecipitated with DDX1 and overexpression of Tat could rescue the unspliced viral mRNA levels inhibited by Nullbasic in HIV-1 expressing cells.

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Host Cell Interactome of HIV-1 Rev Includes RNA Helicases Involved in Multiple Facets of Virus Production

Cited by 118 publications

References 56 publications

Depletion of hnRNP A2/B1 overrides the nuclear retention of the HIV-1 genomic RNA

Depletion of hnRNP A2/B1 overrides the nuclear retention of the HIV-1 genomic RNA

Non-POU Domain-Containing Octamer-Binding Protein Negatively Regulates HIV-1 Infection in CD4⁺T Cells

A HIV-1 Tat mutant protein disrupts HIV-1 Rev function by targeting the DEAD-box RNA helicase DDX1

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Host Cell Interactome of HIV-1 Rev Includes RNA Helicases Involved in Multiple Facets of Virus Production

Cited by 118 publications

References 56 publications

Depletion of hnRNP A2/B1 overrides the nuclear retention of the HIV-1 genomic RNA

Depletion of hnRNP A2/B1 overrides the nuclear retention of the HIV-1 genomic RNA

Non-POU Domain-Containing Octamer-Binding Protein Negatively Regulates HIV-1 Infection in CD4+T Cells

A HIV-1 Tat mutant protein disrupts HIV-1 Rev function by targeting the DEAD-box RNA helicase DDX1

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About

Non-POU Domain-Containing Octamer-Binding Protein Negatively Regulates HIV-1 Infection in CD4⁺T Cells