Antibody Inhibition of a Viral Type 1 Interferon Decoy Receptor Cures a Viral Disease by Restoring Interferon Signaling in the Liver

Xu, Ren Huan; Rubio, Daniel; Roscoe, Felicia; Krouse, Tracy E.; Truckenmiller, M.E.; Norbury, Christopher C.; Hudson, Paul; Damon, Inger K.; Alcamı́, Antonio; Sigal, Luis J.

doi:10.1371/journal.ppat.1002475

Cited by 27 publications

(36 citation statements)

References 61 publications

(84 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Rather, we think that passive immunization temporarily reduces virus loads, allowing the development of active immunity. This is supported by our previous reports that passive transfer of Abs or memory T cells protects only immunocompetent hosts from mousepox (34,43) and a report by Lustig et al showing that VIG does not permanently protect SCID mice from VACV challenge (28).…”

Section: Discussionsupporting

confidence: 78%

“…2g, right). In all cases, the positive-control antiserum to the type I IFN binding protein was protective (34), while naive serum was not. Hence, the data obtained with pAbs confirm that the MV protein EVM072 is a better target for late Ab therapy than the EV proteins EVM135 and EVM155.…”

Section: L1r A33rmentioning

confidence: 90%

“…Our work described here demonstrates that as measured by survival, viral loads, and liver damage, neutralizing Abs to the MV protein L1R/EVM072 are more effective than cometinhibiting Abs to the EV proteins A33R/EVM135 and B5R/ EVM155 at controlling an otherwise lethal ECTV infection when given after viral dissemination to susceptible but otherwise immunocompetent mice. We have recently shown that blocking IgG1 MAbs to B18R/EVM166, which encode a secreted, nonstructural type I interferon decoy receptor, also cures mousepox when administered after viral dissemination (34). While MAb VMC-78 to the EV protein A33R/EVM135 promoted survival when given at 5 dpi, it did not significantly decrease virus loads or liver pathology 2 days after treatment.…”

Section: Discussionmentioning

confidence: 99%

“…Production of recombinant A33R, EVM135, B5R, and EVM155 was as previously described (18,33). Production of polyclonal rabbit antibodies (Abs) was also as previously described (34). MAbs VMC-2, VMC-14, and VMC-78 (all IgG1) have been described previously (33,35) and were either obtained from BEI Resources (Manassas, VA) or produced and purified as described previously (33,35).…”

Section: Methodsmentioning

confidence: 99%

See 3 more Smart Citations

The Mature Virion of Ectromelia Virus, a Pathogenic Poxvirus, Is Capable of Intrahepatic Spread and Can Serve as a Target for Delayed Therapy

Roscoe

et al. 2013

J Virol

Self Cite

View full text Add to dashboard Cite

Orthopoxviruses (OPVs), which include the agent of smallpox (variola virus), the zoonotic monkeypox virus, the vaccine and zoonotic species vaccinia virus, and the mouse pathogen ectromelia virus (ECTV), form two types of infectious viral particles: the mature virus (MV), which is cytosolic, and the enveloped virus (EV), which is extracellular. It is believed that MVs are required for viral entry into the host, while EVs are responsible for spread within the host. Following footpad infection of susceptible mice, ECTV spreads lymphohematogenously, entering the liver at 3 to 4 days postinfection (dpi). Afterwards, ECTV spreads intrahepatically, killing the host. We found that antibodies to an MV protein were highly effective at curing mice from ECTV infection when administered after the virus reached the liver. Moreover, a mutant ECTV that does not make EV was able to spread intrahepatically and kill immunodeficient mice. Together, these findings indicate that MVs are sufficient for the spread of ECTV within the liver and could have implications regarding the pathogenesis of other OPVs, the treatment of emerging OPV infections, as well as strategies for preparedness in case of accidental or intentional release of pathogenic OPVs.

show abstract

Section: Discussionsupporting

confidence: 78%

Section: L1r A33rmentioning

confidence: 90%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

The Mature Virion of Ectromelia Virus, a Pathogenic Poxvirus, Is Capable of Intrahepatic Spread and Can Serve as a Target for Delayed Therapy

Roscoe

et al. 2013

J Virol

Self Cite

View full text Add to dashboard Cite

show abstract

“…The extraction of total RNA from tissue and reverse transcription of RNA were carried out as described previously (36), and the PCR was done as before (37). The following dye combinations were used for detection and data normalization: 6-carboxyfluorescein (FAM) (reporter for IFNs, MX-1, and IL-6) and hexachlorofluorescein (HEX) (reporter for glyceraldehyde-3-phosphate dehydrogenase [GAPDH]).…”

Section: Animalsmentioning

confidence: 99%

MyD88-Dependent Immunity to a Natural Model of Vaccinia Virus Infection Does Not Involve Toll-Like Receptor 2

Davies

Sei

Siciliano

et al. 2014

J Virol

Self Cite

View full text Add to dashboard Cite

Although the pattern recognition receptor Toll-like receptor 2 (TLR2) is typically thought to recognize bacterial components, it has been described to alter the induction of both innate and adaptive immunity to a number of viruses, including vaccinia virus (VACV). However, many pathogens that reportedly encode TLR2 agonists may actually be artifactually contaminated during preparation, possibly with cellular debris or merely with molecules that sensitize cells to be activated by authentic TLR2 agonists. In both humans and mice, the most relevant natural route of infection with VACV is through intradermal infection of the skin. Therefore, we examined the requirement for TLR2 and its signaling adaptor MyD88 in protective immunity to VACV after intradermal infection. We find that although TLR2 may recognize virus preparations in vitro and have a minor role in preventing dissemination of VACV following systemic infection with large doses of virus, it is wholly disposable in both control of virus replication and induction of adaptive immunity following intradermal infection. In contrast, MyD88 is required for efficient induction of CD4 T cell and B cell responses and for local control of virus replication following intradermal infection. However, even MyD88 is not required to induce local inflammation, inflammatory cytokine production, or recruitment of cells that restrict virus from spreading systemically after peripheral infection. Thus, an effective antiviral response does require MyD88, but TLR2 is not required for control of a peripheral VACV infection. These findings emphasize the importance of studying relevant routes of infection when examining innate sensing mechanisms. IMPORTANCEVaccinia virus (VACV) provides the backbone for some of the most widely used and successful viral vaccine vectors and is also related to the human pathogens Cantagalo virus and molluscum contagiosum virus that infect the skin of patients. Therefore, it is vital to understand the mechanisms that induce a strong innate immune response to the virus following dermal infection. Here, we compare the ability of the innate sensing molecule Toll-like receptor 2 (TLR2) and the signaling molecule MyD88 to influence the innate and adaptive immune response to VACV following systemic or dermal infection.

show abstract

Viral pathogen-induced mechanisms to antagonize mammalian interferon (IFN) signaling pathway

Rojas

Alejo

Martı́n

et al. 2020

Cell. Mol. Life Sci.

View full text Add to dashboard Cite

Antiviral responses of interferons (IFNs) are crucial in the host immune response, playing a relevant role in controlling viralw infections. Three types of IFNs, type I (IFN-α, IFN-β), II (IFN-γ) and III (IFN-λ), are classified according to their receptor usage, mode of induction, biological activity and amino acid sequence. Here, we provide a comprehensive review of type I IFN responses and different mechanisms that viruses employ to circumvent this response. In the first part, we will give an overview of the different induction and signaling cascades induced in the cell by IFN-I after virus encounter. Next, highlights of some of the mechanisms used by viruses to counteract the IFN induction will be described. And finally, we will address different mechanism used by viruses to interference with the IFN signaling cascade and the blockade of IFN induced antiviral activities.

show abstract

Antibody Inhibition of a Viral Type 1 Interferon Decoy Receptor Cures a Viral Disease by Restoring Interferon Signaling in the Liver

Cited by 27 publications

References 61 publications

The Mature Virion of Ectromelia Virus, a Pathogenic Poxvirus, Is Capable of Intrahepatic Spread and Can Serve as a Target for Delayed Therapy

The Mature Virion of Ectromelia Virus, a Pathogenic Poxvirus, Is Capable of Intrahepatic Spread and Can Serve as a Target for Delayed Therapy

MyD88-Dependent Immunity to a Natural Model of Vaccinia Virus Infection Does Not Involve Toll-Like Receptor 2

Viral pathogen-induced mechanisms to antagonize mammalian interferon (IFN) signaling pathway

Contact Info

Product

Resources

About