Literature DB >> 18369187

Unexpected roles for UPF1 in HIV-1 RNA metabolism and translation.

Lara Ajamian1, Levon Abrahamyan, Miroslav Milev, Pavel V Ivanov, Andreas E Kulozik, Niels H Gehring, Andrew J Mouland.   

Abstract

The HIV-1 ribonucleoprotein (RNP) contains the major structural protein, pr55(Gag), viral genomic RNA, as well as the host protein, Staufen1. In this report, we show that the nonsense-mediated decay (NMD) factor UPF1 is also a component of the HIV-1 RNP. We investigated the role of UPF1 in HIV-1-expressing cells. Depletion of UPF1 by siRNA resulted in a dramatic reduction in steady-state HIV-1 RNA and pr55(Gag). Pr55(Gag) synthesis, but not the cognate genomic RNA, was efficiently rescued by expression of an siRNA-insensitive UPF1, demonstrating that UPF1 positively influences HIV-1 RNA translatability. Conversely, overexpression of UPF1 led to a dramatic up-regulation of HIV-1 expression at the RNA and protein synthesis levels. The effects of UPF1 on HIV-1 RNA stability were observed in the nucleus and cytoplasm and required ongoing translation. We also demonstrate that the effects exerted by UPF1 on HIV-1 expression were dependent on its ATPase activity, but were separable from its role in NMD and did not require interaction with UPF2.

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Year:  2008        PMID: 18369187      PMCID: PMC2327365          DOI: 10.1261/rna.829208

Source DB:  PubMed          Journal:  RNA        ISSN: 1355-8382            Impact factor:   4.942


  61 in total

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  55 in total

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Review 2.  Nonsense-mediated mRNA decay in human cells: mechanistic insights, functions beyond quality control and the double-life of NMD factors.

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5.  Characterizing HIV-1 Splicing by Using Next-Generation Sequencing.

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Review 7.  The multiple lives of NMD factors: balancing roles in gene and genome regulation.

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9.  Live cell visualization of the interactions between HIV-1 Gag and the cellular RNA-binding protein Staufen1.

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