Essential Role of IL-17A in the Formation of a Mycobacterial Infection-Induced Granuloma in the Lung

Yoshida, Yasuhiko; Umemura, Masayuki; Yahagi, Ayano; O’Brien, Rebecca L.; Ikuta, Koichi; Kishihara, Kenji; Hara, Hiromitsu; Nakae, Susumu; Iwakura, Yoichiro; Matsuzaki, Goro

doi:10.4049/jimmunol.0903332

Cited by 348 publications

(292 citation statements)

References 51 publications

(55 reference statements)

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“…42 This is partially independent of IFN-g and appears to be associated with IL-17-driven granuloma formation. 42,43 Immune protection in Mtb infection is certainly multifaceted; for example, we show here that IL-7 decreased in NHP PBMCs IL-10 and Foxp3 gene expression, whereas only IL-7, yet not IFN-g yielded increased IL-17 gene and protein expression in PBMCs from 5/5 NHPs (Figure 2). Thus, increased IL-17 protein detection in situ and IL-7-driven IL-17 production in vitro suggest that the 6 exonspanning IL-7 protein mediates beneficial effects in Mtb infection via IL-17 induction.…”

Section: Il-mentioning

confidence: 82%

Increased (6 exon) interleukin-7 production after M. tuberculosis infection and soluble interleukin-7 receptor expression in lung tissue

et al. 2011

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Interleukin-7 (IL-7) and the IL-7 receptor (IL-7R) have been shown to be alternatively spliced in infectious diseases. We tested IL-7 and IL-7R splicing in a tuberculosis (TB)-vaccine/Mycobacterium tuberculosis (Mtb)-challenge model in non-human primates (NHPs). Differential IL-7 splicing was detected in peripheral blood mononuclear cells (PBMCs) from 15/15 NHPs showing 6 different IL-7 spliced isoforms. This pattern did not change after infection with virulent Mtb. We demonstrated increased IL-7 (6 exon) and IL-17 protein production in lung tissue along with concomitant decreased transforming growth factor-b (TGF-b) from NHPs (vaccinated with a recombinant BCG (rBCG)) who showed increased survival after Mtb challenge. IL-7 increased IL-17 and interferon-g (IFN-g) gene and protein expression in PBMCs. Mtb-infected NHPs showed differential IL-7R splicing associated with the anatomical location and tissue origin, that is, in lung tissue, hilus, axillary lymph nodes (LNs) and spleen. Differential splicing of the IL-7R was typical for healthy (non-Mtb infected) and for Mtb-infected lung tissue with a dominant expression of soluble IL-7R (sIL-7R) receptor lacking exon 6 (9:1 ratio of sIL-7R/cell-bound IL-7R). Differential ratios of cell-bound vs sIL-7R could be observed in hilus and axillary LNs from Mtb-infected NHPs with an inversed ratio of 1:9 (sIL-7R/cell-bound IL-7R) in spleen and PBMCs. Soluble IL-7R is exclusively present in lung tissue.

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Section: Il-mentioning

confidence: 82%

Increased (6 exon) interleukin-7 production after M. tuberculosis infection and soluble interleukin-7 receptor expression in lung tissue

et al. 2011

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“…Inhibition of IL-10 signaling during BCG vaccination enhances host-generated Ag-specific IFN-g and IL-17A responses (50). IL-17A participates in the protection against M. tuberculosis after vaccination (20) and in the formation of the mycobacterial granuloma (18,19). However, IL-17A is a highly inflammatory cytokine implicated in a number of chronic inflammatory diseases, including TB, and it may be responsible for substantial tissue damage in the host (22).…”

Section: Discussionmentioning

confidence: 99%

“…IL-17A controls granulopoiesis and neutrophil recruitment to sites of inflammation, and is another important player in the context of mycobacterial infections. It is required for granuloma formation after either BCG or M. tuberculosis infection in the mouse (18,19). Th17 memory cells are involved in vaccine-induced protection against M. tuberculosis infection via the rapid recruitment of activated Th1 cells to the lung (20).…”

mentioning

confidence: 99%

Mycobacteria-Infected Dendritic Cells Attract Neutrophils That Produce IL-10 and Specifically Shut Down Th17 CD4 T Cells through Their IL-10 Receptor

Doz

Lombard

Carreras

et al. 2013

The Journal of Immunology

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Neutrophils participate in the control of mycobacterial infection both by directly eliminating bacilli and by interacting with macrophages and dendritic cells (DCs). Despite host defenses, slow-growing mycobacteria can persist in the host for decades, mostly inside macrophages and DCs, and eventually destroy tissues after exacerbated inflammation. IL-17A–driven neutrophil recruitment may participate in this process. We report that mouse bone marrow–derived DCs infected with live Mycobacterium bovis Bacillus Calmette-Guérin (BCG) produced large amounts of CXCL1 and CXCL2, and attracted neutrophils. After physical contact with DCs infected with live BCG, the neutrophils produced large quantities of the immunosuppressive cytokine IL-10 via the MyD88 and spleen tyrosine kinase pathways. The CD11b integrin was involved in this neutrophil–DC interaction and allowed IL-10 production. TCR OVA transgenic mice immunized with a BCG strain producing OVA mounted an OVA-specific Th17 and Th1 CD4 response. Interestingly, IL-10–producing neutrophils specifically shut down IL-17A production by Th17 CD4 cells, but not IFN-γ production by Th1 cells. This was due to Th17 CD4 cell–restricted expression of the receptor for IL-10. After neutrophil depletion, total mouse lung cells produced less IL-10 but more IL-17A; IFN-γ production was not affected. Therefore, we suggest that during mycobacterial infection, regulatory neutrophils are instructed by infected reservoir DCs to produce IL-10 that specifically targets IL-10Rα–expressing Th17 CD4 T cells. This could be important to control the otherwise exuberant Th17 response.

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“…Th17 cells accelerate the accumulation of Th1 cells and enhance Th1 antimycobacterial responses (33)(34)(35). IL-17 also plays a role in the formation and maintenance of granuloma in mycobacteria-infected lungs (36,37). However, re-exposure of tuberculosis-infected mice to high levels of tuberculosis Ag promotes further Th17 responses that cause extensive lung damage associated with elevated neutrophil recruitment (38).…”

Section: Discussionmentioning

confidence: 99%

Role of Th1/Th17 Balance Regulated by T-bet in a Mouse Model of Mycobacterium avium Complex Disease

Matsuyama

Ishii

Yageta

et al. 2014

The Journal of Immunology

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Th1 immune responses are thought to be important in protection against intracellular pathogens. T-bet is a critical regulator for Th1 cell differentiation and Th1 cytokine production. The aim of this study was to determine the role of T-bet in host defense against Mycobacterium avium complex (MAC) infection. Wild-type mice, T-bet–deficient mice, and T-bet–overexpressing mice were infected with MAC via intratracheal inoculation. Macrophages and dendritic cells obtained from these mice were incubated with MAC. T-bet–deficient mice were highly susceptible to MAC, compared with wild-type mice and T-bet–overexpressing mice. Neutrophilic pulmonary inflammation was also enhanced in T-bet–deficient mice, but attenuated in T-bet–overexpressing mice, following MAC infection. Cytokine expression shifted toward Th1 in the lung and spleen of T-bet–overexpressing mice, but toward Th17 in T-bet–deficient mice. IFN-γ supplementation to T-bet–deficient mice reduced systemic MAC growth but did not reduce pulmonary inflammation. In contrast, neutralization of IL-17 in T-bet–deficient mice reduced pulmonary inflammation but did not affect mycobacterial growth in any organs tested. T-bet–deficient T cells tended to differentiate toward Th17 cells in vitro following exposure to MAC. Treatment with NO donor suppressed MAC-induced Th17 cell differentiation of T-bet–deficient T cells. This study identified that the fine balance between Th1 and Th17 responses is essential in defining the outcome of MAC disease. T-bet functions as a regulator for Th1/Th17 balance and is a critical determinant for host resistance to MAC infection by controlling cytokine and NO levels.

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Essential Role of IL-17A in the Formation of a Mycobacterial Infection-Induced Granuloma in the Lung

Cited by 348 publications

References 51 publications

Increased (6 exon) interleukin-7 production after M. tuberculosis infection and soluble interleukin-7 receptor expression in lung tissue

Increased (6 exon) interleukin-7 production after M. tuberculosis infection and soluble interleukin-7 receptor expression in lung tissue

Mycobacteria-Infected Dendritic Cells Attract Neutrophils That Produce IL-10 and Specifically Shut Down Th17 CD4 T Cells through Their IL-10 Receptor

Role of Th1/Th17 Balance Regulated by T-bet in a Mouse Model of Mycobacterium avium Complex Disease

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