Type I IFN Induces IL-10 Production in an IL-27–Independent Manner and Blocks Responsiveness to IFN-γ for Production of IL-12 and Bacterial Killing in <i>Mycobacterium tuberculosis</i>–Infected Macrophages

McNab, Finlay W.; Ewbank, John; Howes, Ashleigh; Moreira-Teixeira, Lúcia; Martirosyan, Anna; Ghilardi, Nico; Saraiva, Margarida; O’Garra, Anne

doi:10.4049/jimmunol.1401088

Cited by 173 publications

(213 citation statements)

References 76 publications

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“…This finding agrees with the literature, where a correlation between IFN-b production and the virulence of W-Beijing strains has been established (Manca et al, 2001;. Moreover, a recent investigation of the association between type I IFN production and bacterial virulence demonstrated a role for type I IFN in inducing the immunosuppressive cytokine IL-10 and in repressing the cytoprotective effect of IFN-g in Mtb-infected macrophages (McNab et al, 2014). These results are consistent with our data, which show both strongly suppressed production of IL-10 and enhanced macrophage survival in cGAS knockout and STING knockout cells.…”

Section: Discussionsupporting

confidence: 89%

Mycobacterium tuberculosis Differentially Activates cGAS- and Inflammasome-Dependent Intracellular Immune Responses through ESX-1

Wassermann

Gulen

Sala

et al. 2015

Cell Host & Microbe

342

330

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Cytosolic detection of microbial products is essential for the initiation of an innate immune response against intracellular pathogens such as Mycobacterium tuberculosis (Mtb). During Mtb infection of macrophages, activation of cytosolic surveillance pathways is dependent on the mycobacterial ESX-1 secretion system and leads to type I interferon (IFN) and interleukin-1β (IL-1β) production. Whereas the inflammasome regulates IL-1β secretion, the receptor(s) responsible for the activation of type I IFNs has remained elusive. We demonstrate that the cytosolic DNA sensor cyclic GMP-AMP synthase (cGAS) is essential for initiating an IFN response to Mtb infection. cGAS associates with Mtb DNA in the cytosol to stimulate cyclic GAMP (cGAMP) synthesis. Notably, activation of cGAS-dependent cytosolic host responses can be uncoupled from inflammasome activation by modulating the secretion of ESX-1 substrates. Our findings identify cGAS as an innate sensor of Mtb and provide insight into how ESX-1 controls the activation of specific intracellular recognition pathways.

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Section: Discussionsupporting

confidence: 89%

Mycobacterium tuberculosis Differentially Activates cGAS- and Inflammasome-Dependent Intracellular Immune Responses through ESX-1

Wassermann

Gulen

Sala

et al. 2015

Cell Host & Microbe

342

330

View full text Add to dashboard Cite

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“…S5B). Results could thus not be ascribed to auto-and paracrine activity of individual cytokines despite the well-characterized importance of these cytokines in mycobacterial defenses (2,3,7,18,39,40). We therefore propose that Keap1 acts as a negative regulator for controlling inflammatory signaling in M. avium-infected human primary macrophages.…”

Section: Discussionmentioning

confidence: 90%

Keap1 regulates inflammatory signaling in Mycobacterium avium -infected human macrophages

Awuh

Haug

Mildenberger

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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Several mechanisms are involved in controlling intracellular survival of pathogenic mycobacteria in host macrophages, but how these mechanisms are regulated remains poorly understood. We report a role for Kelch-like ECH-associated protein 1 (Keap1), an oxidative stress sensor, in regulating inflammation induced by infection with Mycobacterium avium in human primary macrophages. By using confocal microscopy, we found that Keap1 associated with mycobacterial phagosomes in a time-dependent manner, whereas siRNA-mediated knockdown of Keap1 increased M. aviuminduced expression of inflammatory cytokines and type I interferons (IFNs). We show evidence of a mechanism whereby Keap1, as part of an E3 ubiquitin ligase complex with Cul3 and Rbx1, facilitates ubiquitination and degradation of IκB kinase (IKK)-β thus terminating IKK activity. Keap1 knockdown led to increased nuclear translocation of transcription factors NF-κB, IFN regulatory factor (IRF) 1, and IRF5 driving the expression of inflammatory cytokines and IFN-β. Furthermore, knockdown of other members of the Cul3 ubiquitin ligase complex also led to increased cytokine expression, further implicating this ligase complex in the regulation of the IKK family. Finally, increased inflammatory responses in Keap1-silenced cells contributed to decreased intracellular growth of M. avium in primary human macrophages that was reconstituted with inhibitors of IKKβ or TANK-binding kinase 1 (TBK1). Taken together, we propose that Keap1 acts as a negative regulator for the control of inflammatory signaling in M. avium-infected human primary macrophages. Although this might be important to avoid sustained or overwhelming inflammation, our data suggest that a negative consequence could be facilitated growth of pathogens like M. avium inside macrophages.Keap1 | human primary macrophages | infection | Mycobacterium avium | inflammation

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“…S9E). Type I IFNs are known to inhibit IL-12-p70 in myeloid cells, including DCs (27), and in particular in M. tuberculosis-infected monocytes and macrophages (28,29). Accordingly, stimulation by IFNβ resulted in a strong suppression of IL-12-p70 production by TLR2-activated In I, cells were left untreated or were treated with the SHP2 inhibitor GS-493 (24).…”

Section: Dcir Deficiency Results In Enhanced Antimycobacterial Th1 Immentioning

confidence: 99%

C-type lectin receptor DCIR modulates immunity to tuberculosis by sustaining type I interferon signaling in dendritic cells

Troegeler

Mercier

Cougoule

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Immune response against pathogens is a tightly regulated process that must ensure microbial control while preserving integrity of the infected organs. Tuberculosis (TB) is a paramount example of a chronic infection in which antimicrobial immunity is protective in the vast majority of infected individuals but can become detrimental if not finely tuned. Here, we report that C-type lectin dendritic cell (DC) immunoreceptor (DCIR), a key component in DC homeostasis, is required to modulate lung inflammation and bacterial burden in TB. DCIR is abundantly expressed in pulmonary lesions in Mycobacterium tuberculosis-infected nonhuman primates during both latent and active disease. In mice, we found that DCIR deficiency impairs STAT1-mediated type I IFN signaling in DCs, leading to increased production of IL-12 and increased differentiation of T lymphocytes toward Th1 during infection. As a consequence, DCIR-deficient mice control M. tuberculosis better than WT animals but also develop more inflammation characterized by an increased production of TNF and inducible NOS (iNOS) in the lungs. Altogether, our results reveal a pathway by which a C-type lectin modulates the equilibrium between infection-driven inflammation and pathogen’s control through sustaining type I IFN signaling in DCs.

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Type I IFN Induces IL-10 Production in an IL-27–Independent Manner and Blocks Responsiveness to IFN-γ for Production of IL-12 and Bacterial Killing in Mycobacterium tuberculosis–Infected Macrophages

Cited by 173 publications

References 76 publications

Mycobacterium tuberculosis Differentially Activates cGAS- and Inflammasome-Dependent Intracellular Immune Responses through ESX-1

Mycobacterium tuberculosis Differentially Activates cGAS- and Inflammasome-Dependent Intracellular Immune Responses through ESX-1

Keap1 regulates inflammatory signaling in Mycobacterium avium -infected human macrophages

C-type lectin receptor DCIR modulates immunity to tuberculosis by sustaining type I interferon signaling in dendritic cells

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