Ectromelia virus accumulates less double-stranded RNA compared to vaccinia virus in BS-C-1 cells

Frey, Tiffany R.; Lehmann, Michael H.; Ryan, Colton M.; Pizzorno, Marie C.; Sutter, Gerd; Hersperger, Adam R.

doi:10.1016/j.virol.2017.06.010

Cited by 11 publications

(16 citation statements)

References 71 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…With respect to poxviruses, it has been known for some time that vaccinia virus (VACV) forms abundant amounts of dsRNA, especially during intermediate and late time points of the infection cycle (i.e., after DNA replication; “post-replicative”) (Boone et al, 1979; Colby and Duesberg, 1969; Colby et al, 1971; Duesberg and Colby, 1969). Other orthopoxviruses, such as cowpox virus, also form dsRNA albeit to a varying degree relative to VACV (Frey et al, 2017). The mechanism of dsRNA formation has been discussed elsewhere (Arndt et al, 2016; Frey et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

“…Other orthopoxviruses, such as cowpox virus, also form dsRNA albeit to a varying degree relative to VACV (Frey et al, 2017). The mechanism of dsRNA formation has been discussed elsewhere (Arndt et al, 2016; Frey et al, 2017). Briefly, it has been demonstrated using VACV as a model that dsRNA forms as a result of several factors: minimal intergenic space, convergent transcription from opposite DNA strands, and inefficient termination of transcription, particularly during post-replicative time points (Xiang et al, 2000; 1998).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Ectromelia virus lacking the E3L ortholog is replication-defective and nonpathogenic but does induce protective immunity in a mouse strain susceptible to lethal mousepox

et al. 2018

Self Cite

View full text Add to dashboard Cite

All known orthopoxviruses, including ectromelia virus (ECTV), contain a gene in the E3L family. The protein product of this gene, E3, is a double-stranded RNA-binding protein. It can impact host range and is used by orthopoxviruses to combat cellular defense pathways, such as PKR and RNase L. In this work, we constructed an ECTV mutant with a targeted disruption of the E3L open reading frame (ECTVΔE3L). Infection with this virus resulted in an abortive replication cycle in all cell lines tested. We detected limited transcription of late genes but no significant translation of these mRNAs. Notably, the replication defects of ECTVΔE3L were rescued in human and mouse cells lacking PKR. ECTVΔE3L was nonpathogenic in BALB/c mice, a strain susceptible to lethal mousepox disease. However, infection with ECTVΔE3L induced protective immunity upon subsequent challenge with wild-type virus. In summary, E3L is an essential gene for ECTV.

show abstract

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Ectromelia virus lacking the E3L ortholog is replication-defective and nonpathogenic but does induce protective immunity in a mouse strain susceptible to lethal mousepox

et al. 2018

Self Cite

View full text Add to dashboard Cite

show abstract

“…Our procedure was modelled on previous reports [81–83]. HFF and HeLa cells were mock infected or infected with the indicated viruses at MOI 10 for 12 hours.…”

Section: Methodsmentioning

confidence: 99%

The herpes simplex virus host shutoff (vhs) RNase limits accumulation of double stranded RNA in infected cells: Evidence for accelerated decay of duplex RNA

2019

View full text Add to dashboard Cite

The herpes simplex virus virion host shutoff (vhs) RNase destabilizes cellular and viral mRNAs and blunts host innate antiviral responses. Previous work demonstrated that cells infected with vhs mutants display enhanced activation of the host double-stranded RNA (dsRNA)-activated protein kinase R (PKR), implying that vhs limits dsRNA accumulation in infected cells. Confirming this hypothesis, we show that partially complementary transcripts of the UL23/UL24 and UL30/31 regions of the viral genome increase in abundance when vhs is inactivated, giving rise to greatly increased levels of intracellular dsRNA formed by annealing of the overlapping portions of these RNAs. Thus, vhs limits accumulation of dsRNA at least in part by reducing the levels of complementary viral transcripts. We then asked if vhs also destabilizes dsRNA after its initial formation. Here, we used a reporter system employing two mCherry expression plasmids bearing complementary 3’ UTRs to produce defined dsRNA species in uninfected cells. The dsRNAs are unstable, but are markedly stabilized by co-expressing the HSV dsRNA-binding protein US11. Strikingly, vhs delivered by super-infecting HSV virions accelerates the decay of these pre-formed dsRNAs in both the presence and absence of US11, a novel and unanticipated activity of vhs. Vhs binds the host RNA helicase eIF4A, and we find that vhs-induced dsRNA decay is attenuated by the eIF4A inhibitor hippuristanol, providing evidence that eIF4A participates in the process. Our results show that a herpesvirus host shutoff RNase destabilizes dsRNA in addition to targeting partially complementary viral mRNAs, raising the possibility that the mRNA destabilizing proteins of other viral pathogens dampen the host response to dsRNA through similar mechanisms.

show abstract

“…To counteract the host responses to viral dsRNA, viruses either sequester it, degrade it, or interfere with the host cell sensing machinery or effector pathways. Thus, the production of less dsRNA (presumably by minimizing late run-on transcription compared to VACV) can be a strategy for some poxviruses such as MPXV, ECTV, and MYXV to subvert host activation of innate immune responses [ 58 , 59 ]. As an additional measure, these viruses also encode E3-like dsRNA binding proteins ( Figure 2 ).…”

Section: Regulation Of Host Antiviral Signaling Pathwaysmentioning

confidence: 99%

Myxoma Virus-Encoded Host Range Protein M029: A Multifunctional Antagonist Targeting Multiple Host Antiviral and Innate Immune Pathways

Rahman

McFadden

2020

Vaccines

View full text Add to dashboard Cite

Myxoma virus (MYXV) is the prototypic member of the Leporipoxvirus genus of the Poxviridae family of viruses. In nature, MYXV is highly restricted to leporids and causes a lethal disease called myxomatosis only in European rabbits (Oryctologous cuniculus). However, MYXV has been shown to also productively infect various types of nonrabbit transformed and cancer cells in vitro and in vivo, whereas their normal somatic cell counterparts undergo abortive infections. This selective tropism of MYXV for cancer cells outside the rabbit host has facilitated its development as an oncolytic virus for the treatment of different types of cancers. Like other poxviruses, MYXV possesses a large dsDNA genome which encodes an array of dozens of immunomodulatory proteins that are important for host and cellular tropism and modulation of host antiviral innate immune responses, some of which are rabbit-specific and others can function in nonrabbit cells as well. This review summarizes the functions of one such MYXV host range protein, M029, an ortholog of the larger superfamily of poxvirus encoded E3-like dsRNA binding proteins. M029 has been identified as a multifunctional protein involved in MYXV cellular and host tropism, antiviral responses, and pathogenicity in rabbits.

show abstract

Ectromelia virus accumulates less double-stranded RNA compared to vaccinia virus in BS-C-1 cells

Cited by 11 publications

References 71 publications

Ectromelia virus lacking the E3L ortholog is replication-defective and nonpathogenic but does induce protective immunity in a mouse strain susceptible to lethal mousepox

Ectromelia virus lacking the E3L ortholog is replication-defective and nonpathogenic but does induce protective immunity in a mouse strain susceptible to lethal mousepox

The herpes simplex virus host shutoff (vhs) RNase limits accumulation of double stranded RNA in infected cells: Evidence for accelerated decay of duplex RNA

Myxoma Virus-Encoded Host Range Protein M029: A Multifunctional Antagonist Targeting Multiple Host Antiviral and Innate Immune Pathways

Contact Info

Product

Resources

About