Transcriptional Analysis of Murine Macrophages Infected with Different Toxoplasma Strains Identifies Novel Regulation of Host Signaling Pathways

Melo, Mariane B.; Nguyen, Quynh; Cordeiro, Cynthia Azeredo; Hassan, Musa A.; Yang, Ninghan; McKell, Renee; Rosowski, Emily E.; Julien, Lindsay; Butty, Vincent; Dardé, Marie‐Laure; Ajzenberg, Daniel; Fitzgerald, Katherine A.; Young, Lucy H.; Saeij, Jeroen P. J.

doi:10.1371/journal.ppat.1003779

Cited by 87 publications

(108 citation statements)

References 82 publications

(109 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…T . gondii infection, moreover, does not elicit type 1 IFNs and their potential disease-exacerbating comorbidities [33]; a phenomenon observed in the course of many infections and an important consideration, particularly in the context of STAT2 deficiency and hence disrupted type 1 IFN signaling [34]. At first, WT- and STAT2-deficient mice were injected with IFN-γ or PBS (controls), before peritoneal macrophages were collected for ex vivo infection experiments with T .…”

Section: Resultsmentioning

confidence: 99%

STAT2 Is a Pervasive Cytokine Regulator due to Its Inhibition of STAT1 in Multiple Signaling Pathways

Pelzel

Begitt

et al. 2016

PLoS Biol

View full text Add to dashboard Cite

STAT2 is the quintessential transcription factor for type 1 interferons (IFNs), where it functions as a heterodimer with STAT1. However, the human and murine STAT2-deficient phenotypes suggest important additional and currently unidentified type 1 IFN-independent activities. Here, we show that STAT2 constitutively bound to STAT1, but not STAT3, via a conserved interface. While this interaction was irrelevant for type 1 interferon signaling and STAT1 activation, it precluded the nuclear translocation specifically of STAT1 in response to IFN-γ, interleukin-6 (IL-6), and IL-27. This is explained by the dimerization between activated STAT1 and unphosphorylated STAT2, whereby the semiphosphorylated dimers adopted a conformation incapable of importin-α binding. This, in turn, substantially attenuated cardinal IFN-γ responses, including MHC expression, senescence, and antiparasitic immunity, and shifted the transcriptional output of IL-27 from STAT1 to STAT3. Our results uncover STAT2 as a pervasive cytokine regulator due to its inhibition of STAT1 in multiple signaling pathways and provide an understanding of the type 1 interferon-independent activities of this protein.

show abstract

Section: Resultsmentioning

confidence: 99%

STAT2 Is a Pervasive Cytokine Regulator due to Its Inhibition of STAT1 in Multiple Signaling Pathways

Pelzel

Begitt

et al. 2016

PLoS Biol

View full text Add to dashboard Cite

show abstract

“…In support of this hypothesis, it has been shown that T. gondii infection of fibroblasts pre-stimulated with IFNγ triggers a stronger type I IFN response than infection of untreated fibroblasts 35 . ISG-encoded GTPases are essential for controlling the infection both ex vivo 42,44 and in vivo, as mice lacking genes of the IRG family or genes encoding several GBPs are more susceptible to T. gondii infection than their wild-type counterparts 42,[45][46][47] .…”

mentioning

confidence: 88%

“…1c) in macrophages infected with less virulent T. gondii type II strains but not in macrophages infected with virulent type I strains 60 . This protein is highly polymorphic, and differences in its amino acid sequence and its expression levels seem to explain the variations observed between distinct T. gondii strains concerning the activation of pro-inflammatory host genes 35 . GRA15 is secreted from dense granules and traffics to the host cytosol during the invasion and intracellular growth of PV-enclosed T. gondii parasites.…”

Section: Bacterial Pathogensmentioning

confidence: 99%

“…This pathogen not only triggers the NAIP-NLRC4 pathway via the T3SS 6,7 , but also activates the NOD2 pathway 22 , a GBPdependent signalling pathway (resulting in caspase 11 activation) 24 and GAL8-induced autophagy 68 . Similarly, not only is T. gondii recognized through the reduction in IRGMs on the PV and the detection of effectors in the cytosol, but this pathogen also triggers inflammasome activation, and some non-canonical T. gondii strains induce a type I IFN response by exposing dsRNA to RIG-I or endosomal TLRs 26,35,61,[64][65][66] . This emerging appreciation for the complexity of mechanisms involved in the detection of a given pathogen will probably also expand the complexity of the analyses required for their study, as it will be crucial to carefully discriminate between the effects of the different modes of innate immune activation.…”

Section: Many Means Complexity By Combinationmentioning

confidence: 99%

“…Their detection could be mediated by the cell in two ways: first, by inducing a loss of vacuolar-membrane integrity and subsequent leakage of pathogen ligands into the cytosol, where they activate cytosolic receptors; or second, by regaining control over the PV, prompting either vacuole acidification and endolyso somal fusion or a cellular autophagic response against the pathogen, which in both cases leads to pathogen ligands being accessible to endosomal TLRs 34 . These recognition mechanisms might occur for two closely related apicomplexan parasites: T. gondii and N. caninum 35,36 .…”

mentioning

confidence: 99%

See 2 more Smart Citations

Unveiling the pathogen behind the vacuole

Liehl¹,

Zuzarte‐Luís²,

Mota³

2015

Nat Rev Microbiol

View full text Add to dashboard Cite

Many clinically relevant pathogens, including certain bacteria and protozoan parasites, have developed an intracellular lifestyle that enables them to nestle in customized vacuoles. Although these pathogens are protected from extracellular defences, recent findings indicate that host cells have evolved multiple strategies to unmask the pathogen disguised by the vacuole and thereby initiate innate immune responses. In this Opinion article, we propose and discuss models by which hosts can sense 'professional' vacuolar pathogens, and we highlight the ability of the host to target these stealthy bacteria and parasites.

show abstract

Transcriptomic analysis of global changes in cytokine expression in mouse spleens following acute Toxoplasma gondii infection

He¹,

Song³

et al. 2015

Parasitol Res

View full text Add to dashboard Cite

Toxoplasma gondii is a global pathogen that infects a wide range of animals and humans. During T. gondii infection, the spleen plays an important role in coordinating the adaptive and innate immune responses. However, there is little information regarding the changes in global gene expression within the spleen following T. gondii infection. To address this gap in knowledge, we examined the transcriptome of the mouse spleen following T. gondii infection. We observed differential expression of 2310 transcripts under these conditions. Analysis of KEGG and GO enrichment indicated that T. gondii alters multiple immune signaling cascades. Most of differentially expressed GO terms and pathways were downregulated, while immune-related GO terms and pathways were upregulated with response to T. gondii infection in mouse spleen. Most cytokines were upregulated in infected spleens, and all differentially expressed chemokines were upregulated which enhanced the immune cells chemotaxis to promote recruitment of immune cells, such as neutrophils, eosinophils, monocytes, dendritic cells, macrophages, NK cells, basophils, B cells, and T cells. Although IFN-γ-induced IDO (Ido1) was upregulated in the present study, it may not contribute a lot to the control of T. gondii because most differentially expressed genes involved in tryptophan metabolism pathway were downregulated. Innate immunity pathways, including cytosolic nucleic acid sensing pathway and C-type lectins-Syk-Card9 signaling pathways, were upregulated. We believe our study is the first comprehensive attempt to define the host transcriptional response to T. gondii infection in the mouse spleen.

show abstract

Transcriptional Analysis of Murine Macrophages Infected with Different Toxoplasma Strains Identifies Novel Regulation of Host Signaling Pathways

Cited by 87 publications

References 82 publications

STAT2 Is a Pervasive Cytokine Regulator due to Its Inhibition of STAT1 in Multiple Signaling Pathways

STAT2 Is a Pervasive Cytokine Regulator due to Its Inhibition of STAT1 in Multiple Signaling Pathways

Unveiling the pathogen behind the vacuole

Transcriptomic analysis of global changes in cytokine expression in mouse spleens following acute Toxoplasma gondii infection

Contact Info

Product

Resources

About