Th17 Polarization under Hypoxia Results in Increased IL-10 Production in a Pathogen-Independent Manner

Volchenkov, Roman; Nygaard, Vegard; Sener, Zeynep; Skålhegg, Bjørn Steen

doi:10.3389/fimmu.2017.00698

Cited by 20 publications

(19 citation statements)

References 59 publications

(88 reference statements)

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“…To this end, our group and others have investigated whether BCG vaccination of infants has the same effect on the innate immune response. Jensen et al in a cohort of West African infants and our group in United Kingdom infants both showed evidence of enhanced innate responses to non-specific stimuli following infant BCG vaccination ( 89 , 90 ).…”

Section: Dissecting Immune Responses To Bcg At the Cellular And Molecmentioning

confidence: 60%

What Have We Learnt about BCG Vaccination in the Last 20 Years?

2017

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A number of new tuberculosis (TB) vaccines have been or are entering clinical trials, which include genetically modified mycobacteria, mycobacterial antigens delivered by viral vectors, or mycobacterial antigens in adjuvant. Some of these vaccines aim to replace the existing BCG vaccine but others will be given as a boosting vaccine following BCG vaccination given soon after birth. It is clear that the existing BCG vaccines provide incomplete and variable protection against pulmonary TB. This review will discuss what we have learnt over the last 20 years about how the BCG vaccine induces specific and non-specific immunity, what factors influence the immune responses induced by BCG, and progress toward identifying correlates of immunity against TB from BCG vaccination studies. There is still a lot to learn about the BCG vaccine and the insights gained can help the development of more protective vaccines.

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Section: Dissecting Immune Responses To Bcg At the Cellular And Molecmentioning

confidence: 60%

What Have We Learnt about BCG Vaccination in the Last 20 Years?

2017

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“…In tumors, hypoxia can promote development of immunosuppressive microenvironment by affecting the rapid differentiation of myeloid‐derived suppressive cells to tumor‐associated macrophages . Furthermore hypoxic conditions can regulate T cell metabolism and differentiation and Treg (iTreg) and Th17 cell balance, and the regulation of those processes is coordinated by HIF1‐α, RORγ and FoxP3 …”

Section: Introductionmentioning

confidence: 99%

On the relationship between VDR, RORα and RORγ receptors expression and HIF1‐α levels in human melanomas

Brożyna

Jóźwicki

Jetten

et al. 2019

Experimental Dermatology

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We analysed the correlation between the expression of HIF‐1α (hypoxia‐inducible factor 1 alpha), the nuclear receptors: VDR (vitamin D receptor), RORα (retinoic acid receptor‐related orphan receptor alpha), and RORγ and CYP24A1 (cytochrome P450 family 24 subfamily A member 1) and CYP27B1 (cytochrome P450 family 27 subfamily B member 1), enzymes involved in vitamin D metabolism. In primary and metastatic melanomas, VDR negatively correlated with nuclear HIF‐1α expression (r = −.2273, P = .0302; r = −.5081, P = .0011). Furthermore, the highest HIF‐1α expression was observed in pT3‐pT4 VDR‐negative melanomas. A comparative analysis of immunostained HIF‐1α and CYP27B1 and CYP24A1 showed lack of correlation between these parameters both in primary tumors and melanoma metastases. In contrast, RORα expression correlated positively with nuclear HIF‐1α expression in primary and metastatic lesions (r = .2438, P = .0175; r = .3662, P = .0166). Comparable levels of HIF‐1α expression pattern was observed in localized and advanced melanomas. RORγ in primary melanomas correlated also positively with nuclear HIF‐1α expression (r = .2743, P = .0129). HIF‐1α expression was the lowest in localized RORγ‐negative melanomas. In addition, HIF‐1α expression correlated with RORγ‐positive lymphocytes in melanoma metastases. We further found that in metastatic lymph nodes FoxP3 immunostaining correlated positively with HIF‐1α and RORγ expression in melanoma cells (r = .3667; P = .0327; r = .4208, P = .0129). In summary, our study indicates that the expression of VDR, RORα and RORγ in melanomas is related to hypoxia and/or HIF1‐α activity, which also affects FoxP3 expression in metastatic melanoma. Therefore, the hypoxia can affect tumor biology by changing nuclear receptors expression and molecular pathways regulated by nuclear receptors and immune responses.

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“…Significant functional and morphologic differences between the nephritic groups were not found at the examined time point, whereas profound differences were demonstrated in intrarenal T h 17 cells. We reason this discrepancy to be related to the pathogenic functional impairment of renal infiltrating T h 17 cells, as has been shown recently by others (37) and should be further addressed in the NTN model.…”

Section: Discussionmentioning

confidence: 50%

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model

et al. 2018

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Experimental nephrotoxic serum nephritis (NTN) is a model for T‐cell–mediated human rapid progressive glomerulonephritis. T‐cell receptor stimulation involves intracellular signaling events that ultimately lead to the activation of transcription factors, such as NF‐κB. We explored the involvement of the NF‐κB components IKK‐2 and NEMO in NTN, by using cell‐specific knockouts of IKK‐2 and NEMO in CD4+ T lymphocytes. Our results demonstrate that although the course of disease was not grossly altered in CD4xIKK2Δ and CD4xNEMOΔ animals, renal regulatory T cells were significantly reduced and T helper (Th)1 and Th17 cells significantly increased in both knockout mouse groups. The expression of the renal cytokines and chemokines IL‐1β, CCL‐2, and CCL‐20 was also significantly altered in both knockout mice. Lymphocyte transcriptome analysis confirmed the increased expression of Th17‐related cytokines in spleen CD4+ T cells. Moreover, our array data demonstrate an interrupted canonical NF‐κB pathway and an increased expression of noncanonical NF‐κB pathway–related genes in nephritic CD4xNEMOΔ mice, highlighting different downstream effects of deletion of IKK‐2 or NEMO in T lymphocytes. We propose that better understanding of the role of IKK‐2 and NEMO in nephritis is essential for the clinical application of kinase inhibitors in patients with glomerulonephritis.—Guo, L., Huang, J., Chen, M., Piotrowski, E., Song, N., Zahner, G., Paust, H.‐J., Alawi, M., Geffers, R., Thaiss, F. T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces Th17 cells in an experimental nephrotoxic nephritis mouse model. FASEB J. 33, 2359–2371 (2019). http://www.fasebj.org

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Th17 Polarization under Hypoxia Results in Increased IL-10 Production in a Pathogen-Independent Manner

Cited by 20 publications

References 59 publications

What Have We Learnt about BCG Vaccination in the Last 20 Years?

What Have We Learnt about BCG Vaccination in the Last 20 Years?

On the relationship between VDR, RORα and RORγ receptors expression and HIF1‐α levels in human melanomas

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model

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Th17 Polarization under Hypoxia Results in Increased IL-10 Production in a Pathogen-Independent Manner

Cited by 20 publications

References 59 publications

What Have We Learnt about BCG Vaccination in the Last 20 Years?

What Have We Learnt about BCG Vaccination in the Last 20 Years?

On the relationship between VDR, RORα and RORγ receptors expression and HIF1‐α levels in human melanomas

T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T h 17 cells in an experimental nephrotoxic nephritis mouse model

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T‐lymphocyte–specific knockout of IKK‐2 or NEMO induces T _h 17 cells in an experimental nephrotoxic nephritis mouse model