Insufficient IL-10 Production as a Mechanism Underlying the Pathogenesis of Systemic Juvenile Idiopathic Arthritis

Imbrechts, Maya; Avau, Anneleen; Vandenhaute, Jessica; Malengier‐Devlies, Bert; Put, Karen; Mitera, Tania; Berghmans, Nele; Burton, Oliver T.; Junius, Steffie; Liston, Adrian; Somer, Lien De; Wouters, Carine; Matthys, Patrick

doi:10.4049/jimmunol.1800468

Cited by 24 publications

(19 citation statements)

References 50 publications

(70 reference statements)

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“…In fact, 2 independent studies in systemic JIA cohorts showed increased prevalence of IL10 promoter haplotypes that encode for low IL-10 expression (83,84). Recently, cell-specific IL-10 defects were observed in patients with systemic JIA and in a murine disease model, resulting in insufficient IL-10 production to counterbalance proinflammatory cytokines (85).…”

Section: Fromautoinflammationtoautoimmunitymentioning

confidence: 99%

Innately Adaptive or Truly Autoimmune: Is There Something Unique About Systemic Juvenile Idiopathic Arthritis?

Kessel

Hedrich

Foell

2020

Arthritis & Rheumatology

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Systemic juvenile idiopathic arthritis (JIA) is a form of arthritis in childhood that is initially dominated by innate immunity-driven systemic inflammation and is thus considered a polygenic autoinflammatory disease. However, systemic JIA can progress toward an adaptive immunity-driven afebrile arthritis. Based on this observation of biphasic disease progression, a "window of opportunity" for optimal, individualized and target-directed treatment has been proposed. This hypothesis requires testing, and in this review we summarize current evidence regarding molecular factors that may contribute to the progression from an initially predominantly autoinflammatory disease phenotype to autoimmune arthritis. We consider the involvement of innately adaptive γδ T cells and natural killer T cells that express γδ or αβ T cell receptors but cannot be classified as either purely innate or adaptive cells, versus classic B and T lymphocytes in this continuum. Finally, we discuss our understanding of how and why some primarily autoinflammatory conditions can progress toward autoimmune-mediated disorders over the disease course while others do not and how this knowledge may be used to offer individualized treatment.Dr. Foell's work was supported by the DFG (project FO 354/11-1).

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Section: Fromautoinflammationtoautoimmunitymentioning

confidence: 99%

Innately Adaptive or Truly Autoimmune: Is There Something Unique About Systemic Juvenile Idiopathic Arthritis?

Kessel

Hedrich

Foell

2020

Arthritis & Rheumatology

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“…Arthritis was not observed in the experiments, most likely because the mice were sacrificed before onset of arthritis [joint inflammation is a late feature seen in CFA-challenged IFN-g KO mice (21)]. A parameter that may predict the potential development of arthritis is the formation of TRAP + -multinucleated osteoclasts ex vivo as described by Imbrechts et al (24). Splenocytes were stimulated with osteoclastdifferentiating factor RANKL and M-CSF, and after 7 d the osteoclasts were stained for TRAP.…”

Section: Resultsmentioning

confidence: 99%

“…For differentiation to osteoclasts, the cells were incubated with receptor activator of NF-kB ligand (RANKL; 100 ng/ml; R&D Systems) and M-CSF (20 ng/ml; R&D Systems). After 3 d, the cells were restimulated with fresh medium and stimuli for 3-4 d, followed by staining of the cells for tartrate-resistant acid phosphatase (TRAP) as described (23,24).…”

Section: Histologic and Cytospin Analyses Cell Isolation And Enrichmentioning

confidence: 99%

Regulatory Role for NK Cells in a Mouse Model of Systemic Juvenile Idiopathic Arthritis

Vandenhaute

Avau

Filtjens

et al. 2019

The Journal of Immunology

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Mice deficient in IFN-g (IFN-g knockout [KO] mice) develop a systemic inflammatory syndrome in response to CFA, in contrast to CFA-challenged wild-type (WT) mice who only develop a mild inflammation. Symptoms in CFA-challenged IFN-g KO resemble systemic juvenile idiopathic arthritis (sJIA), a childhood immune disorder of unknown cause. Dysregulation of innate immune cells is considered to be important in the disease pathogenesis. In this study, we used this murine model to investigate the role of NK cells in the pathogenesis of sJIA. NK cells of CFA-challenged IFN-g KO mice displayed an aberrant balance of activating and inhibitory NK cell receptors, lower expression of cytotoxic proteins, and a defective NK cell cytotoxicity. Depletion of NK cells (via anti-IL-2Rb and anti-Asialo-GM1 Abs) or blockade of the NK cell activating receptor NKG2D in CFA-challenged WT mice resulted in increased severity of systemic inflammation and appearance of sJIA-like symptoms. NK cells of CFA-challenged IFN-g KO mice and from anti-NKG2D-treated mice showed defective degranulation capacities toward autologous activated immune cells, predominantly monocytes. This is in line with the increased numbers of activated inflammatory monocytes in these mice which was particularly reflected in the expression of CCR2, a chemokine receptor, and in the expression of Rae-1, a ligand for NKG2D. In conclusion, NK cells are defective in a mouse model of sJIA and impede disease development in CFA-challenged WT mice. Our findings point toward a regulatory role for NK cells in CFA-induced systemic inflammation via a NKG2D-dependent control of activated immune cells.

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“…In a study published by Imbrechts et al, experimental evidence was provided on a mouse model that there would be a relationship between IL-10 insufficient production and its consequence in the innate cellular immune response from sJIA pathogenesis [58].…”

Section: Molecular and Cellular Mechanisms Of Systemic Arthritismentioning

confidence: 99%

Molecular and Cellular Mechanisms of Arthritis in Children and Adults: New Perspectives on Applied Photobiomodulation

Ailioaie

Litscher

2020

IJMS

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Juvenile idiopathic arthritis and adult rheumatoid arthritis are two major groups with chronic joint pain and inflammation, extra-articular manifestations, and high risk of comorbidities, which can cause physical and ocular disability, as well as create great socio-economic pressure worldwide. The pathogenesis of arthritis manifested in childhood and adulthood is multifactorial, unclear, and overly complex, in which immunity plays an important role. Although there are more and more biological agents with different mechanisms of action for the treatment of arthritis, the results are not as expected, because there are partial responses or non-responsive patients to these compounds, high therapeutic costs, side effects, and so on; therefore, we must turn our attention to other therapeutic modalities. Updating knowledge on molecular and cellular mechanisms in the comparative pathogenesis of chronic arthritis in both children and adults is necessary in the early and correct approach to treatment. Photobiomodulation (PBM) represents a good option, offering cost-effective advantages over drug therapy, with a quicker, more positive response to treatment and no side effects. The successful management of PBM in arthritis is based on the clinician’s ability to evaluate correctly the inflammatory status of the patient, to seek the optimal solution, to choose the best technology with the best physical parameters, and to select the mode of action to target very precisely the immune system and the molecular signaling pathways at the molecular level with the exact amount of quantum light energy in order to obtain the desired immune modulation and the remission of the disease. Light is a very powerful tool in medicine because it can simultaneously target many cascades of immune system activation in comparison with drugs, so PBM can perform very delicate tasks inside our cells to modulate cellular dysfunctions, helping to initiate self-organization phenomena and finally, healing the disease. Interdisciplinary teams should work diligently to meet these needs by also using single-cell imaging devices for multispectral laser photobiomodulation on immune cells.

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Insufficient IL-10 Production as a Mechanism Underlying the Pathogenesis of Systemic Juvenile Idiopathic Arthritis

Cited by 24 publications

References 50 publications

Innately Adaptive or Truly Autoimmune: Is There Something Unique About Systemic Juvenile Idiopathic Arthritis?

Innately Adaptive or Truly Autoimmune: Is There Something Unique About Systemic Juvenile Idiopathic Arthritis?

Regulatory Role for NK Cells in a Mouse Model of Systemic Juvenile Idiopathic Arthritis

Molecular and Cellular Mechanisms of Arthritis in Children and Adults: New Perspectives on Applied Photobiomodulation

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