Translational resistance of late alphavirus mRNA to eIF2α phosphorylation: a strategy to overcome the antiviral effect of protein kinase PKR

Ventoso, Iván; Sanz, Miguel Á.; Molina, Susana; Berlanga, Juan José; Carrasco, Luís; Esteban, Mariano

doi:10.1101/gad.357006

Cited by 180 publications

(309 citation statements)

References 59 publications

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“…Although the response in locally treated tumors was fast and strong, it was still insufficient to prevent virus replication and subsequent tumor cell destruction. Alphaviruses, including SFV, are known to resist IFN response, as they can slow down protein translation via formation of specific capsid RNA haipin structures, 29 which allows viral replication in the presence of active PKR. On the other hand, despite the slower onset of the IFN response in the i.v.-treated animals, the antitumor effect of the vector administered systemically was more modest.…”

Section: Discussionmentioning

confidence: 99%

Evaluation of cancer virotherapy with attenuated replicative Semliki forest virus in different rodent tumor models

Määttä

Liimatainen

Wahlfors

et al. 2007

Intl Journal of Cancer

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Semliki Forest virus (SFV) is one of the latest candidates for a virotherapeutic agent against cancer, and recent studies have demonstrated its efficacy in tumor models. In the present study, we examined the antitumor efficacy of an avirulent SFV strain A7(74) and its derivative, a replication-competent SFV vector VA7-EGFP, in a partially immunodeficient mouse tumor model (subcutaneous A549 human lung adenocarcinoma in NMRI nu/nu mouse) and in an immunocompetent rat tumor model (intracranial BT4C glioma in BDIX rat). When subcutaneous mouse tumors were injected 3 times with VA7-EGFP, intratumorally treated animals showed almost complete inhibition of tumor growth, while systemically treated mice displayed only delayed tumor growth (intravenous injection) or no response at all (intraperitoneal injection). This was at least partially due to a strong type I interferon (IFN) response in the tumors. The animals did not display any signs of abnormal behavior or encephalitis, even though SFV-positive foci were detected in the brain after the initial blood viremia. Intracranial rat tumors were injected directly with SFV A7(74) virus and monitored with magnetic resonance imaging. Tumor growth was significantly reduced (p < 0.05) with one virus injection, but the tumor size continued to increase after a lag period and none of the treated animals survived. Three virus injections or T-cell suppression with dexamethasone did not significantly improve treatment efficacy. It appeared that the local virotherapy induced extensive production of neutralizing anti-SFV antibodies that most likely contributed to the insufficient treatment efficacy. In conclusion, we show here that SFV A7(74) is a potential oncolytic agent for cancer virotherapy, but major immunological hurdles may need to be overcome before the virus can be clinically tested. ' 2007 Wiley-Liss, Inc.

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Section: Discussionmentioning

confidence: 99%

Evaluation of cancer virotherapy with attenuated replicative Semliki forest virus in different rodent tumor models

Määttä

Liimatainen

Wahlfors

et al. 2007

Intl Journal of Cancer

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“…respectively, as compared with their counterparts that bear the viral DLP structure (SV-DLP Luc and SV-DLP EGFP). No differences in expression were detected in PKR o/o cells, showing that phosphorylation of eIF2 hampered translation of nonviral mRNAs as described before (22). Next, we quantified the extent of translational exclusion of EGFP mRNA in SV-infected cells compared with cellular mRNAs (e.g., β-actin).…”

Section: Engineered Reporter Mrnas That Mimic Translation Of Cellularmentioning

confidence: 99%

“…A DLP structure included in the first 90 nts of the 26S mRNA coding sequence was also placed in the indicated reporter mRNAs. In SV-ΔDLP EGFP the secondary structure of DLP was disrupted by point mutations as described previously (22) …”

Section: Engineered Reporter Mrnas That Mimic Translation Of Cellularmentioning

confidence: 99%

“…A remarkable exception to this are the members of alphavirus group (Sindbis and Semliki Forest virus). Thus, complete phosphorylation of eIF2 was found in cultured mouse fibroblasts infected with these viruses, so that only viral mRNA is translated under these circumstances (22,29). The presence of a secondary structure, termed downstream hairpin loop (DLP) and located 27 nts downstream from the initiator AUG in viral 26S transcripts, allows this mRNA to be translated by an eIF2-independent mechanism in infected cells (22,30).…”

mentioning

confidence: 99%

“…Another important point of translation control in infected cells relies on the activity of eIF2 that brings the initiator Met-tRNA to 40S ribosomes (20)(21)(22)(23). In response to viral infection, host dsRNAactivated kinase (PKR) phosphorylates eIF2 in an attempt to block general translation (both cellular and viral) (24)(25)(26)(27).…”

mentioning

confidence: 99%

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Inhibition of host translation by virus infection in vivo

Toribio

Ventoso

2010

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

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Infection of cultured cells with lytic animal viruses often results in the selective inhibition of host protein synthesis, whereas viral mRNA is efficiently translated under these circumstances. This phenomenon, known as "shut off," has been well described at the molecular level for some viruses, but there is not yet any direct or indirect evidence supporting the idea that it also should operate in animals infected with viruses. To address this issue, we constructed recombinant Sindbis virus (SV)-expressing reporter mRNA, the translation of which is sensitive or resistant to virus-induced shut off. As found in cultured cells, replication of SV in mouse brain was associated with a strong phosphorylation of eukaryotic initiation factor (eIF2) that prevented translation of reporter mRNA (luciferase and EGFP). Translation of these reporters was restored in vitro, in vivo, and ex vivo when a viral RNA structure, termed downstream hairpin loop, present in viral 26S mRNA, was placed at the 5′ end of reporter mRNAs. By comparing the expression of shut off-sensitive and -resistant reporters, we unequivocally concluded that replication of SV in animal tissues is associated with a profound inhibition of nonviral mRNA translation. A strategy as simple as that followed here might be applicable to other viruses to evaluate their interference on host translation in infected animals.eukaryotic initiation factor-2 phosphorylation | dsRNA-dependent protein kinase | Sindbis

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Regulation of stress granules and P‐bodies during RNA virus infection

2013

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RNA granules are structures within cells that play major roles in gene expression and homeostasis. Two principle kinds of RNA granules are conserved from yeast to mammals: stress granules (SGs), which contain stalled translation initiation complexes, and processing bodies (P-bodies, PBs), which are enriched with factors involved in RNA turnover. Since RNA granules are associated with silenced transcripts, viruses subvert RNA granule function for replicative advantages. This review, focusing on RNA viruses, discusses mechanisms that manipulate stress granules and P-bodies to promote synthesis of viral proteins. Three main themes have emerged for how viruses manipulate RNA granules; i) cleavage of key host factors, ii) control of PKR activation and iii) redirecting RNA granule components for new or parallel roles in viral reproduction, at the same time disrupting RNA granules. Viruses utilize one or more of these routes to achieve robust and productive infection.

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Translational resistance of late alphavirus mRNA to eIF2α phosphorylation: a strategy to overcome the antiviral effect of protein kinase PKR

Cited by 180 publications

References 59 publications

Evaluation of cancer virotherapy with attenuated replicative Semliki forest virus in different rodent tumor models

Evaluation of cancer virotherapy with attenuated replicative Semliki forest virus in different rodent tumor models

Inhibition of host translation by virus infection in vivo

Regulation of stress granules and P‐bodies during RNA virus infection

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