Interferon-Independent Innate Responses to Cytomegalovirus

Ashley, Caroline L; Abendroth, Allison; McSharry, Brian P.; Slobedman, Barry

doi:10.3389/fimmu.2019.02751

Cited by 47 publications

(38 citation statements)

References 172 publications

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“…Moreover, mCherry high and low cells display distinct antiviral gene signatures ( Fig 1D ). While the genes analyzed in this study are designated as interferon-simulated genes (ISGs), IFN-independent upregulation by virus replication of some of these genes has been described [ 22 – 24 ] and we do not distinguish between virus induced and interferon induced. The putative protective ISGs found in the mCherry low cells at 12 hpi overlap with the genes identified using both ΔHA-mCherry and ΔHA-destabilized GFP at 24 hpi identified previously [ 14 ] ( Fig 1E , top, S1 Table ).…”

Section: Resultsmentioning

confidence: 99%

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Cell type- and replication stage-specific influenza virus responses in vivo

et al. 2020

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Influenza A viruses (IAVs) remain a significant global health burden. Activation of the innate immune response is important for controlling early virus replication and spread. It is unclear how early IAV replication events contribute to immune detection. Additionally, while many cell types in the lung can be infected, it is not known if all cell types contribute equally to establish the antiviral state in the host. Here, we use single-cycle influenza A viruses (scIAVs) to characterize the early immune response to IAV in vitro and in vivo. We found that the magnitude of virus replication contributes to antiviral gene expression within infected cells prior to the induction of a global response. We also developed a scIAV that is only capable of undergoing primary transcription, the earliest stage of virus replication. Using this tool, we uncovered replication stage-specific responses in vitro and in vivo. Using several innate immune receptor knockout cell lines, we identify RIG-I as the predominant antiviral detector of primary virus transcription and amplified replication in vitro. Through a Cre-inducible reporter mouse, we used scIAVs expressing Cre-recombinase to characterize cell typespecific responses in vivo. Individual cell types upregulate unique sets of antiviral genes in response to both primary virus transcription and amplified replication. We also identified antiviral genes that are only upregulated in response to direct infection. Altogether, these data offer insight into the early mechanisms of antiviral gene activation during influenza A infection.

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Section: Resultsmentioning

confidence: 99%

“…IFN-independent, IRF-dependent upregulation of some ISGs has been described [ 22 – 24 ]. In these studies, detection of viral RNA products is still required for virus-induced gene expression.…”

Section: Discussionmentioning

confidence: 99%

Cell type- and replication stage-specific influenza virus responses in vivo

et al. 2020

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“…For instance, recent work by the Mü hlberger lab showed that MARV VP35 inhibits PKR in human but not ERB cells, and there is precedent for IFN-independent response induction by IRF3 or STAT1 of subsets of canonical antiviral genes during in vitro human cytomegalovirus (HCMV) infection. [40][41][42] This does not preclude, however, the alternative possibilities that induction of IFN gene transcription simply occurs at levels too low for nCounter to detect, certain IFN proteins are activated on a post-transcriptional level, and/or the ability of MARV proteins to fully suppress IFN is cell type-dependent, any of which would suggest that IFNs still act as master antiviral response regulators in MARV-infected ERBs, perhaps in a paracrine fashion, without a need for noncanonical explanations. Of most relevance to pathogenesis among the cytokine/chemokine non-DEGs in ERBs is that they appear to be largely pro-or ambi-inflammatory; several are highly induced in primate filoviral infections, including IFNg, IL2, IL4, MIP-1b (CCL4), and CSF2.…”

Section: Article Discussionmentioning

confidence: 99%

Asymptomatic Infection of Marburg Virus Reservoir Bats Is Explained by a Strategy of Immunoprotective Disease Tolerance

et al. 2021

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“…Unlike other classical components of innate immunity, they are constitutively expressed within the host cells and are generally IFN inducible, thus allowing an immediate response against viral infection through specific targeting of viral/cellular components (Bieniasz, 2003;Hotter and Kirchhoff, 2018). Interestingly, during HCMV infection a subset of classical IFN-stimulated genes (ISGs) may be also induced or upregulated independently of IFN (Ashley et al, 2019).…”

Section: Restriction Factors Vs Hcmv: a Never Ending Fightmentioning

confidence: 99%

Tuning the Orchestra: HCMV vs. Innate Immunity

et al. 2020

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Understanding how the innate immune system keeps human cytomegalovirus (HCMV) in check has recently become a critical issue in light of the global clinical burden of HCMV infection in newborns and immunodeficient patients. Innate immunity constitutes the first line of host defense against HCMV as it involves a complex array of cooperating effectors -e.g., inflammatory cytokines, type I interferon (IFN-I), natural killer (NK) cells, professional antigen-presenting cells (APCs) and phagocytes -all capable of disrupting HCMV replication. These factors are known to trigger a highly efficient adaptive immune response, where cellular restriction factors (RFs) play a major gatekeeping role. Unlike other innate immunity components, RFs are constitutively expressed in many cell types, ready to act before pathogen exposure. Nonetheless, the existence of a positive regulatory feedback loop between RFs and IFNs is clear evidence of an intimate cooperation between intrinsic and innate immunity. In the course of virushost coevolution, HCMV has, however, learned how to manipulate the functions of multiple cellular players of the host innate immune response to achieve latency and persistence. Thus, HCMV acts like an orchestra conductor able to piece together and rearrange parts of a musical score (i.e., innate immunity) to obtain the best live performance (i.e., viral fitness). It is therefore unquestionable that innovative therapeutic solutions able to prevent HCMV immune evasion in congenitally infected infants and immunocompromised individuals are urgently needed. Here, we provide an up-to-date review of the mechanisms regulating the interplay between HCMV and innate immunity, focusing on the various strategies of immune escape evolved by this virus to gain a fitness advantage.

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Interferon-Independent Innate Responses to Cytomegalovirus

Cited by 47 publications

References 172 publications

Cell type- and replication stage-specific influenza virus responses in vivo

Cell type- and replication stage-specific influenza virus responses in vivo

Asymptomatic Infection of Marburg Virus Reservoir Bats Is Explained by a Strategy of Immunoprotective Disease Tolerance

Tuning the Orchestra: HCMV vs. Innate Immunity

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