Type I IFN Receptor Regulates Neutrophil Functions and Innate Immunity to <i>Leishmania</i> Parasites

Luo, Xin; Vargas-Inchaustegui, Diego A.; Raimer, S.; Kelly, Brent; Hu, Jiping; Zhu, Leiyi; Sun, Jiaren; Soong, Lynn

doi:10.4049/jimmunol.0903273

Cited by 84 publications

(84 citation statements)

References 54 publications

(71 reference statements)

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“…Other studies of protozoan parasite infections suggest a requirement for IFN-I in mediating innate and adaptive immune responses [38][39][40]. Our study is the first to demonstrate that IFN-I impedes primary, adaptive immune responses during infection with a protozoan parasite.…”

Section: Discussionsupporting

confidence: 58%

“…By employing IFN-aR1 À/À mice, which are deficient in IFN-I signalling, we clearly showed that IFN-I indirectly suppressed CD4 1 T-cell responses during blood-stage infection, and impeded control of parasites in two different murine blood-stage malaria models. IFN-I are known to play a crucial role in protection against viruses [36,37], but their role in Plasmodium infections and other protozoan parasite infections has not been extensively studied [38][39][40]. The role of IFN-I during blood-stage Plasmodium infection is not clear, although early studies detected IFN activity in the blood after Plasmodium infection [41].…”

Section: Discussionmentioning

confidence: 99%

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Type I interferons suppress CD4⁺ T‐cell‐dependent parasite control during blood‐stage Plasmodium infection

et al. 2011

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During blood‐stage Plasmodium infection, large‐scale invasion of RBCs often occurs before the generation of cellular immune responses. In Plasmodium berghei ANKA (PbA)‐infected C57BL/6 mice, CD4+ T cells controlled parasite numbers poorly, instead providing early help to pathogenic CD8+ T cells. Expression analysis revealed that the transcriptional signature of CD4+ T cells from PbA‐infected mice was dominated by type I IFN (IFN‐I) and IFN‐γ‐signalling pathway‐related genes. A role for IFN‐I during blood‐stage Plasmodium infection had yet to be established. Here, we observed IFN‐α protein production in the spleen of PbA‐infected C57BL/6 mice over the first 2 days of infection. Mice deficient in IFN‐I signalling had reduced parasite burdens, and displayed none of the fatal neurological symptoms associated with PbA infection. IFN‐I substantially inhibited CD4+ T‐bet+ T‐cell‐derived IFN‐γ production, and prevented this emerging Th1 response from controlling parasites. Experiments using BM chimeric mice revealed that IFN‐I signalled predominantly via radio‐sensitive, haematopoietic cells, but did not suppress CD4+ T cells via direct signalling to this cell type. Finally, we found that IFN‐I suppressed IFN‐γ production, and hampered efficient control of parasitaemia in mice infected with non‐lethal Plasmodium chabaudi. Thus, we have elucidated a novel regulatory pathway in primary blood‐stage Plasmodium infection that suppresses CD4+ T‐cell‐mediated parasite control.

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Section: Discussionsupporting

confidence: 58%

Section: Discussionmentioning

confidence: 99%

Type I interferons suppress CD4⁺ T‐cell‐dependent parasite control during blood‐stage Plasmodium infection

et al. 2011

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“…We have shown that L. amazonensis parasites induce IFN1-b expression via RNAdependent protein kinase (PKR) in a TLR2-dependent manner (3) and that IFN1-b favors parasite growth. In addition, IFN1-a receptor (IFNAR) signaling favors L. amazonensis infection in mice (4). Another component of host immune defense subverted by L. amazonensis is the reactive oxygen species (ROS) defense mechanism.…”

mentioning

confidence: 99%

The integrated endoplasmic reticulum stress response in Leishmania amazonensis macrophage infection: the role of X‐box binding protein 1 transcription factor

et al. 2015

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Endoplasmic reticulum (ER) stress triggers the integrated ER-stress response (IERSR) that ensures cellular survival of ER stress and represents a primordial form of innate immunity. We investigated the role of IERSR during Leishmania amazonensis infection. Treatment of RAW 264.7 infected macrophages with the ER stress-inducing agent thapsigargin (TG; 1 mM) increased L. amazonensis infectivity in an IFN1-a receptor (IFNAR)-dependent manner. In Western blot assays, we showed that L. amazonensis activates the inositol-requiring enzyme (IRE1)/ X-box binding protein (XBP)-1-splicing arms of the IERSR in host cells. In chromatin immunoprecipitation (ChIP) assays, we showed an increased occupancy of enhancer and promoter sequences for the Ifnb gene by XBP1 in infected RAW 264.7 cells. Knocking down XBP1 expression by transducing RAW 264.7 cells with the short hairpin XBP1 lentiviral vector significantly reduced the parasite proliferation associated with impaired translocation of phosphorylated IFN regulatory transcription factor (IRF)-3 to the nucleus and a decrease in IFN1-b expression. Knocking down XBP1 expression also increased NO concentration, as determined by Griess reaction and reduced the expression of antioxidant genes, such as heme oxygenase (HO)-1, that protect parasites from oxidative stress. We conclude that L. amazonensis activation of XBP1 plays a critical role in infection by protecting the parasites from oxidative stress and increasing IFN1-b expression.-

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“…Treatment of infected human macrophages with poly I:C promotes parasite replication in a PKR-dependent manner, although the role of type I IFN was not formally established. In vivo, L. amazonensis-infected Ifnar1 2/2 mice show reduced parasite load, as well as decreased pathology, compared with WT mice (152). The increased resistance is associated with enhanced recruitment of neutrophils.…”

Section: Leishmaniamentioning

confidence: 97%

“…The increased resistance is associated with enhanced recruitment of neutrophils. In this case, neutrophils are believed to mediate pathogen killing by releasing enzymes, such as elastase and myeloperoxidase (152).…”

Section: Leishmaniamentioning

confidence: 99%

Interfering with Immunity: Detrimental Role of Type I IFNs during Infection

Stifter¹,

Feng²

2015

The Journal of Immunology

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Type I IFNs are known to inhibit viral replication and mediate protection against viral infection. However, recent studies revealed that these cytokines play a broader and more fundamental role in host responses to infections beyond their well-established antiviral function. Type I IFN induction, often associated with microbial evasion mechanisms unique to virulent microorganisms, is now shown to increase host susceptibility to a diverse range of pathogens, including some viruses. This article presents an overview of the role of type I IFNs in infections with bacterial, fungal, parasitic, and viral pathogens and discusses the key mechanisms mediating the regulatory function of type I IFNs in pathogen clearance and tissue inflammation.

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Type I IFN Receptor Regulates Neutrophil Functions and Innate Immunity to Leishmania Parasites

Cited by 84 publications

References 54 publications

Type I interferons suppress CD4⁺ T‐cell‐dependent parasite control during blood‐stage Plasmodium infection

Type I interferons suppress CD4⁺ T‐cell‐dependent parasite control during blood‐stage Plasmodium infection

The integrated endoplasmic reticulum stress response in Leishmania amazonensis macrophage infection: the role of X‐box binding protein 1 transcription factor

Interfering with Immunity: Detrimental Role of Type I IFNs during Infection

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Type I IFN Receptor Regulates Neutrophil Functions and Innate Immunity to Leishmania Parasites

Cited by 84 publications

References 54 publications

Type I interferons suppress CD4+ T‐cell‐dependent parasite control during blood‐stage Plasmodium infection

Type I interferons suppress CD4+ T‐cell‐dependent parasite control during blood‐stage Plasmodium infection

The integrated endoplasmic reticulum stress response in Leishmania amazonensis macrophage infection: the role of X‐box binding protein 1 transcription factor

Interfering with Immunity: Detrimental Role of Type I IFNs during Infection

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Type I interferons suppress CD4⁺ T‐cell‐dependent parasite control during blood‐stage Plasmodium infection

Type I interferons suppress CD4⁺ T‐cell‐dependent parasite control during blood‐stage Plasmodium infection