Your search keyword '"van de Loo, Fons A"' showing total 14 results

1. Local inhibition of TGF-β1 signaling improves Th17/Treg balance but not joint pathology during experimental arthritis.

Author

Aarts J, van Caam A, Chen X, Marijnissen RJ, Helsen MM, Walgreen B, Vitters EL, van de Loo FA, van Lent PL, van der Kraan PM, and Koenders MI

Subjects

Animals, Benzodioxoles pharmacology, Cell Differentiation drug effects, Female, Humans, Imidazoles pharmacology, Interleukin-17 metabolism, Mice, Mice, Inbred C57BL, Nuclear Receptor Subfamily 1, Group F, Member 3 metabolism, Pyridines pharmacology, Signal Transduction, T-Lymphocytes, Regulatory drug effects, Th17 Cells drug effects, Tissue Culture Techniques methods, Arthritis, Experimental metabolism, Cytokines metabolism, T-Lymphocytes, Regulatory metabolism, Th17 Cells metabolism, Transforming Growth Factor beta1 metabolism

Abstract

TGF-β1 is an important growth factor to promote the differentiation of T helper 17 (Th17) and regulatory T cells (Treg). The potential of TGF-β1 as therapeutic target in T cell-mediated diseases like rheumatoid arthritis (RA) is unclear. We investigated the effect of TGF-β1 inhibition on murine Th17 differentiation in vitro, on human RA synovial explants ex vivo, and on the development of experimental arthritis in vivo. Murine splenocytes were differentiated into Th17 cells, and the effect of the TGF-βRI inhibitor SB-505124 was studied. Synovial biopsies were cultured in the presence or absence of SB-505124. Experimental arthritis was induced in C57Bl6 mice and treated daily with SB-505124. Flow cytometry analysis was performed to measure different T cell subsets. Histological sections were analysed to determine joint inflammation and destruction. SB-505124 potently reduced murine Th17 differentiation by decreasing Il17a and Rorc gene expression and IL-17 protein production. SB-505124 significantly suppressed IL-6 production by synovial explants. In vivo, SB-505124 reduced Th17 numbers, while increased numbers of Tregs were observed. Despite this skewed Th17/Treg balance, SB-505124 treatment did not result in suppression of joint inflammation and destruction. Blocking TGF-β1 signalling suppresses Th17 differentiation and improves the Th17/Treg balance. However, local SB-505124 treatment does not suppress experimental arthritis., (© 2022. The Author(s).)

Published

2022

2. The in-vivo use of superparamagnetic iron oxide nanoparticles to detect inflammation elicits a cytokine response but does not aggravate experimental arthritis.

Author

Vermeij EA, Koenders MI, Bennink MB, Crowe LA, Maurizi L, Vallée JP, Hofmann H, van den Berg WB, van Lent PL, and van de Loo FA

Subjects

Animals, Arthritis, Experimental pathology, Cytokines genetics, Injections, Intra-Articular, Injections, Intravenous, Magnetic Resonance Imaging, Magnetite Nanoparticles chemistry, Mice, Polyvinyl Alcohol chemistry, Arthritis, Experimental immunology, Cytokines metabolism, Ferric Compounds metabolism, Magnetite Nanoparticles administration & dosage

Abstract

Background: Superparamagnetic Iron Oxide Nanoparticles (SPION) are used in diagnostic imaging of a variety of different diseases. For such in-vivo application, an additional coating with a polymer, for example polyvinyl alcohol (PVA), is needed to stabilize the SPION and prevent aggregation. As the particles are foreign to the body, reaction against the SPION could occur. In this study we investigated the effects that SPION may have on experimental arthritis after intra-articular (i.a.) or intravenous (i.v.) injection., Methods: PVA-coated SPION were injected either i.a. (6 or 24 μg iron) or i.v. (100 μg or 1 mg iron) into naïve Toll-like receptor-4 deficient (TLR4-/-) or wild-type C57Bl/6 mice, or C57Bl/6 mice with antigen-induced arthritis. As control, some mice were injected with PVA or PBS. MR imaging was performed at 1 and 7 days after injection. Mice were sacrificed 2 hours and 1, 2, 7, 10 and 14 days after injection of the SPION, and RNA from synovium and liver was isolated for pro-inflammatory gene expression analysis. Serum cytokine measurements and whole knee joint histology were also performed., Results: Injection of a high dose of SPION or PVA into naïve knee joints resulted in an immediate upregulation of pro-inflammatory gene expression in the synovium. A similar gene expression profile was observed after SPION or PVA injection into knee joints of TLR4-/- mice, indicating that this effect is not due to LPS contamination. Histological analysis of the knee joints also revealed synovial inflammation after SPION injection. Two hours after i.v. injection of SPION or PVA into naïve mice, an upregulation of pro-inflammatory gene expression was detected in the liver. Administration of SPION or PVA into arthritic mice via i.a. injection did not result in an upregulation in gene expression and also no additional effects were observed on histology. MR imaging and histology showed long-term retention of SPION in the inflamed joint. However, 14 days after the injections no long-term effects were evident for gene expression, histology or serum cytokine concentrations., Conclusions: Injection of SPION, either locally or systemically, gives an acute inflammatory response. In the long term, up to 14 days after the injection, while the SPION reside in the joint, no further activating effects of SPION were observed. Hence, we conclude that SPION do not aggravate arthritis and can therefore be used safely to detect joint inflammation by MR imaging.

Published

2015

3. Anticytokine treatment of established type II collagen-induced arthritis in DBA/1 mice: a comparative study using anti-TNFalpha, anti-IL-1alpha/beta and IL-1Ra.

Author

Joosten LA, Helsen MM, van de Loo FA, and van den Berg WB

Subjects

Animals, Antirheumatic Agents pharmacology, Arthritis, Experimental drug therapy, Cytokines immunology, Disease Models, Animal, History, 20th Century, Interleukin-1alpha history, Interleukin-1alpha immunology, Interleukin-1beta history, Interleukin-1beta immunology, Mice, Mice, Inbred DBA, Tumor Necrosis Factor-alpha history, Tumor Necrosis Factor-alpha immunology, Antirheumatic Agents history, Arthritis, Experimental history, Cytokines history

Abstract

Objective: To examine the role of tumor necrosis factor alpha (TNF alpha), interleukin-1 alpha (IL-1 alpha), and IL-1 beta in collagen-induced arthritis (CIA), immediately after onset and during the phase of established arthritis., Methods: Male DBA/1 mice with collagen-induced arthritis were treated with antibodies against murine TNF alpha and IL-1 alpha/beta at different time points of the disease. IL-1 receptor antagonist (IL-1Ra) was administered using Alzet osmotic minipumps. The effect of anticytokine treatment was monitored by visual scoring. Histology and cytokine reverse transcription polymerase chain reaction (RT-PCR) analyses were performed at the end of the treatment period., Results: Anti-TNF alpha treatment showed efficacy shortly after onset of the disease, but had little effect on fully established CIA. Histologic analysis after early treatment revealed that anti-TNF alpha significantly reduced joint pathology, as determined by infiltration of inflammatory cells and cartilage damage. Anti-IL-1 alpha/beta treatment ameliorated both early and full-blown CIA. This clear suppression of established arthritis was confirmed by administration of high doses of IL-1Ra. Dose-response experiments showed that a continuous supply of 1 mg/day was needed for optimal suppression. Histologic analysis showed markedly reduced cartilage destruction both in the knee and the ankle joints. Autoradiography demonstrated full recovery of chondrocyte synthetic function of articular cartilage. In addition, we found that the IL-1 beta isoform plays a dominant role in established CIA. Profound suppression of CIA was observed with anti-IL-1 beta, although elimination of both IL-1 alpha and IL-1 beta still gave better protection. Analysis of messenger RNA with RT-PCR revealed that IL-1 beta was highly upregulated in synovium and cartilage at late stages of CIA, whereas anti-IL-1 beta treatment markedly reduced IL-1 beta message in the synovium., Conclusion: The present study identified different TNF alpha/IL-1 dependencies in various stages of CIA and revealed that blocking of TNF alpha does not necessarily eliminate IL-1. Continuous, high doses of IL-1Ra are needed to block CIA.

Published

2008

4. Role of induced nitric oxide in the initiation of the inflammatory response after postischemic injury.

Author

Cuzzocrea S, Chatterjee PK, Mazzon E, Dugo L, De Sarro A, Van de Loo FA, Caputi AP, and Thiemermann C

Subjects

Animals, Cytokines analysis, Disease Models, Animal, Immunohistochemistry, Inflammation Mediators analysis, Ischemia metabolism, Ischemia mortality, Lipid Peroxidation, Male, Malondialdehyde analysis, Mesenteric Arteries, Mesenteric Vascular Occlusion metabolism, Mesenteric Vascular Occlusion mortality, Mice, Mice, Knockout, Neutrophil Infiltration, Nitric Oxide analysis, Nitric Oxide Synthase analysis, P-Selectin analysis, Peroxidase analysis, Reperfusion Injury metabolism, Reperfusion Injury physiopathology, Sensitivity and Specificity, Survival Rate, Cytokines metabolism, Ischemia pathology, Mesenteric Vascular Occlusion pathology, Nitric Oxide metabolism, Nitric Oxide Synthase metabolism

Abstract

The aim of this study was to investigate the role of inducible nitric oxide (NO) synthase (iNOS) and NO on the modulation of the inflammatory response caused by splanchnic ischemia and reperfusion. A severe model of mesenteric ischemia and reperfusion was produced by subjecting mice to 45 min occlusion followed by reperfusion of the superior mesenteric artery and celiac trunk. In this experimental protocol, wild-type mice treated with GW274150 (5 mg/kg i.p.), a novel, potent, and selective inhibitor of iNOS activity, and mice lacking of the gene for iNOS (iNOS 'knock-out', iNOS-KO) exhibited no difference in the rate of mortality in comparison with wild-type control mice. In a second study, using a less severe model of mesenteric injury obtained by occlusion of the superior mesenteric artery only for 45 min, we evaluated the survival rate. Under these conditions, wild-type mice treated with GW274150 and iNOS-KO mice showed a significant difference in the rate of mortality in comparison with wild-type. Therefore, wild-type mice treated with GW274150 and iNOS-KO mice when compared with wild-type littermates showed a significant reduction of the mesenteric injury, upregulation of P-selectin and intercellular adhesion molecule-1, and neutrophil infiltration, as well as a significant inhibition of the degree of oxidative and nitrosative damage, indicated by malondialdehyde levels, formation of nitrotyrosine and poly(ADP-ribose)polymerase (PARP), respectively. Plasma levels of the proinflammatory cytokines tumour necrosis factor-alpha, interleukin (IL) 6, and IL-1beta were also significantly reduced in iNOS-KO mice in comparison with control wild-type mice. Wild-type mice treated with GW274150 and iNOS-KO mice were also found to have reduced activation of the transcriptional factor nuclear factor-kappaB in the ileum. These results suggest that the induction of iNOS and NO production are essential for the upregulation of the inflammatory response in splanchnic ischemia/reperfusion and participate in end organ damage under these conditions.

Published

2002

5. Inflammation-dependent secretion and splicing of IL-32γ in rheumatoid arthritis

Author

Heinhuis, Bas, Koenders, Marije I., van de Loo, Fons A., Netea, Mihai G., van den Berg, Wim B., Joosten, Leo A. B., and Dinarello, Charles A.

Published

2011

6. IL-32, a Proinflammatory Cytokine in Rheumatoid Arthritis

Author

Joosten, Leo A. B., Netea, Mihai G., Kim, Soo-Hyun, Yoon, Do-Young, Oppers-Walgreen, Birgitte, Radstake, Timothy R. D., Barrera, Pilar, van de Loo, Fons A. J., Dinarello, Charles A., and van den Berg, Wim B.

Published

2006

7. IL37 dampens the IL1β-induced catabolic status of human OA chondrocytes.

Author

van Geffen, Ellen W., van Caam, Arjan P. M., van Beuningen, Henk M., Vitters, Elly L., Schreurs, Wim, van de Loo, Fons A., van Lent, Peter L. E. M., Koenders, Marije I., Blaney Davidson, Esmeralda N., and van der Kraan, Peter M.

Subjects

BIOPSY, CARTILAGE cells, CYTOKINES, IMMUNOHISTOCHEMISTRY, INFLAMMATION, INTERLEUKINS, OSTEOARTHRITIS, STATISTICS, SYNOVIAL membranes, T-test (Statistics), DATA analysis, ONE-way analysis of variance

Abstract

Objective. A crucial feature of OA is cartilage degradation. This process is mediated by pro-inflammatory cytokines, among other factors, via induction of matrix-degrading enzymes. Interleukin 37 (IL37) is an anti-inflammatory cytokine and is efficient in blocking the production of pro-inflammatory cytokines during innate immune responses. We hypothesize that IL37 is therapeutic in treating the inflammatory cytokine cascade in human OA chondrocytes and can act as a counter-regulatory cytokine to reduce cartilage degradation in OA. Methods. Human OA cartilage was obtained from patients undergoing total knee or hip arthroplasty. Immunohistochemistry was applied to study IL37 protein expression in cartilage biopsies from OA patients. Induction of IL37 expression by IL1β, OA synovium-conditioned medium and TNFα was investigated in human OA chondrocytes. Adenoviral overexpression of IL37 followed by IL1β stimulation was performed to investigate the anti-inflammatory potential of IL37. Results. IL37 expression was detected in cartilage biopsies of OA patients and induced by IL1β. After IL1β stimulation, increased IL1β, IL6 and IL8 expression was observed in OA chondrocytes. Elevated IL37 levels diminished the IL1β-induced IL1β, IL6 and IL8 gene levels and IL1β and IL8 protein levels. In addition to the reduction in pro-inflammatory cytokine expression, IL37 reduced MMP1, MMP3, MMP13 and disintegrin and metalloproteinase with thrombospondin motifs 5 gene levels and MMP3 and MMP13 protein levels. Conclusion. IL37 is induced by IL1β, and IL37 itself reduced IL1β, IL6 and IL8 production, indicating that IL37 is able to induce a counter-regulatory anti-inflammatory feedback loop in chondrocytes. In addition, IL37 dampens catabolic enzyme expression. This supports IL37 as a potential therapeutic target in OA. [ABSTRACT FROM AUTHOR]

Published

2017

8. Higher efficacy of anti-IL-6/IL-21 combination therapy compared to monotherapy in the induction phase of Th17-driven experimental arthritis.

Author

Roeleveld, Debbie M., Marijnissen, Renoud J., Walgreen, Birgitte, Helsen, Monique M., van den Bersselaar, Liduine, van de Loo, Fons A., van Lent, Peter L., van der Kraan, Peter M., van den Berg, Wim B., and Koenders, Marije I.

Subjects

INTERLEUKIN-6, T helper cells, TREATMENT of arthritis, JOINT physiology, TRANSFORMING growth factors

Abstract

Th17 cells and their cytokines are linked to the pathogenesis of rheumatoid arthritis, a chronic autoimmune disease characterized by joint inflammation. Th17 development is initiated by combined signaling of TGF-β and IL-6 or IL-21, and can be reduced in the absence of either IL-6 or IL-21. The aim of this study was to assess whether combinatorial IL-6/IL-21 blockade would more potently inhibit Th17 development, and be more efficacious in treating arthritis than targeting either cytokine. We assessed in vitro Th17 differentiation efficacy in the absence of IL-6 and/or IL-21. To investigate in vivo effects of IL-6/IL-21 blockade on Th17 and arthritis development, antigen-induced arthritis (AIA) was induced in IL-6-/- x IL-21R-/- mice. The therapeutic potential of this combined blocking strategy was assessed by treating mice with collagen-induced arthritis (CIA) with anti-IL-6R antibodies and soluble (s)IL-21R.Fc. We demonstrated that combined IL-6/IL-21 blocking synergistically reduced in vitro Th17 differentiation. In mice with AIA, absence of IL-6 and IL-21 signaling more strongly reduced Th17 levels and resulted in stronger suppression of arthritis than the absence of either cytokine. Additionally, anti-IL-6/anti-IL-21 treatment of CIA mice during the arthritis induction phase reduced disease development more potent than IL-6 or IL-21 inhibition alone, as effective as anti-TNF treatment. Collectively, these results suggest dual IL-6/IL-21 inhibition may be a more efficacious therapeutic strategy compared to single cytokine blockade to suppress arthritis development. [ABSTRACT FROM AUTHOR]

Published

2017

9. Functional Tissue Analysis Reveals Successful Cryopreservation of Human Osteoarthritic Synovium.

Author

Broeren, Mathijs G. A., de Vries, Marieke, Bennink, Miranda B., van Lent, Peter L. E. M., van der Kraan, Peter M., Koenders, Marije I., Thurlings, Rogier M., and van de Loo, Fons A. J.

Subjects

SYNOVITIS, CRYOPRESERVATION of organs, tissues, etc., OSTEOARTHRITIS, CRYOPROTECTIVE agents, DISEASE progression, SEVERITY of illness index

Abstract

Osteoarthritis (OA) is a degenerative joint disease affecting cartilage and is the most common form of arthritis worldwide. One third of OA patients have severe synovitis and less than 10% have no evidence of synovitis. Moreover, synovitis is predictive for more severe disease progression. This offers a target for therapy but more research on the pathophysiological processes in the synovial tissue of these patients is needed. Functional studies performed with synovial tissue will be more approachable when this material, that becomes available by joint replacement surgery, can be stored for later use. We set out to determine the consequences of slow-freezing of human OA synovial tissue. Therefore, we validated a method that can be applied in every routine laboratory and performed a comparative study of five cryoprotective agent (CPA) solutions. To determine possible deleterious cryopreservation-thaw effects on viability, the synovial tissue architecture, metabolic activity, RNA quality, expression of cryopreservation associated stress genes, and expression of OA characteristic disease genes was studied. Furthermore, the biological activity of the cryopreserved tissue was determined by measuring cytokine secretion induced by the TLR ligands lipopolysaccharides and Pam3Cys. Compared to non frozen synovium, no difference in cell and tissue morphology could be identified in the conditions using the CS10, standard and CryoSFM CPA solution for cryopreservation. However, we observed significantly lower preservation of tissue morphology with the Biofreeze and CS2 media. The other viability assays showed trends in the same direction but were not sensitive enough to detect significant differences between conditions. In all assays tested a clearly lower viability was detected in the condition in which synovium was frozen without CPA solution. This detailed analysis showed that OA synovial tissue explants can be cryopreserved while maintaining the morphology, viability and phenotypical response after thawing, offering enhanced opportunities for human in vitro studies. [ABSTRACT FROM AUTHOR]

Published

2016

10. Tumor Necrosis Factor, but Not Neutrophils, Alters the Metabolic Profile in Acute Experimental Arthritis.

Author

Oliveira, Marina C., Tavares, Luciana P., Vago, Juliana P., Batista, Nathália V., Queiroz-Junior, Celso M., Vieira, Angelica T., Menezes, Gustavo B., Sousa, Lirlândia P., van de Loo, Fons A. J., Teixeira, Mauro M., Amaral, Flávio A., and Ferreira, Adaliene V. M.

Subjects

TUMOR necrosis factors, NEUTROPHILS, EXPERIMENTAL arthritis, METABOLIC disorders, CYTOKINES

Abstract

Metabolic alterations are associated with arthritis apart from obesity. However, it is still unclear which is the underlying process behind these metabolic changes. Here, we investigate the role of tumor necrosis factor (TNF) in this process in an acute model of antigen-induced arthritis (AIA). Immunized male BALB/c mice received an intra-articular injection of PBS (control) or methylated bovine serum albumin (mBSA) into their knees, and were also pre-treated with different drugs: Etanercept, an anti-TNF drug, DF2156A, a CXCR1/2 receptor antagonist, or a monoclonal antibody RB6-8C5 to deplete neutrophils. Local challenge with mBSA evoked an acute neutrophil influx into the knee joint, and enhanced the joint nociception, along with a transient systemic metabolic alteration (higher levels of glucose and lipids, and altered adipocytokines). Pre-treatment with the conventional biological Etanercept, an inhibitor of TNF action, ameliorated the nociception and the acute joint inflammation dominated by neutrophils, and markedly improved many of the altered systemic metabolites (glucose and lipids), adipocytokines and PTX3. However, the lessening of metabolic changes was not due to diminished accumulation of neutrophils in the joint by Etanercept. Reduction of neutrophil recruitment by pre-treating AIA mice with DF2156A, or even the depletion of these cells by using RB6-8C5 reduced all of the inflammatory parameters and hypernociception developed after AIA challenge, but could not prevent the metabolic changes. Therefore, the induction of joint inflammation provoked acute metabolic alterations which were involved with TNF. We suggest that the role of TNF in arthritis-associated metabolic changes is not due to local neutrophils, which are the major cells present in this model, but rather due to cytokines. [ABSTRACT FROM AUTHOR]

Published

2016

11. Intravenous Delivery of HIV-Based Lentiviral Vectors Preferentially Transduces F4/80+ and Ly-6C+ Cells in Spleen, Important Target Cells in Autoimmune Arthritis.

Author

van den Brand, Ben T., Vermeij, Eline A., Waterborg, Claire E. J., Arntz, Onno J., Kracht, Michael, Bennink, Miranda B., van den Berg, Wim B., and van de Loo, Fons A. J.

Subjects

HIV, SPLEEN, ARTHRITIS, ANTIGEN presenting cells, GENE expression, TRANSGENE expression, LENTIVIRUSES, GREEN fluorescent protein, IMMUNOREGULATION

Abstract

Antigen presenting cells (APCs) play an important role in arthritis and APC specific gene therapeutic targeting will enable intracellular modulation of cell activity. Viral mediated overexpression is a potent approach to achieve adequate transgene expression levels and lentivirus (LV) is useful for sustained expression in target cells. Therefore, we studied the feasibility of lentiviral mediated targeting of APCs in experimental arthritis. Third generation VSV-G pseudotyped self-inactivating (SIN)-LV were injected intravenously and spleen cells were analyzed with flow cytometry for green fluorescent protein (GFP) transgene expression and cell surface markers. Collagen-induced arthritis (CIA) was induced by immunization with bovine collagen type II in complete Freund's adjuvant. Effect on inflammation was monitored macroscopically and T-cell subsets in spleen were analyzed by flow cytometry. Synovium from arthritic knee joints were analyzed for proinflammatory cytokine expression. Lentiviruses injected via the tail vein preferentially infected the spleen and transduction peaks at day 10. A dose escalating study showed that 8% of all spleen cells were targeted and further analysis showed that predominantly Ly6C+ and F4/80+ cells in spleen were targeted by the LV. To study the feasibility of blocking TAK1-dependent pathways by this approach, a catalytically inactive mutant of TAK1 (TAK1-K63W) was overexpressed during CIA. LV-TAK1-K63W significantly reduced incidence and arthritis severity macroscopically. Further histological analysis showed a significant decrease in bone erosion in LV-TAK1-K63W treated animals. Moreover, systemic Th17 levels were decreased by LV-TAK1-K63W treatment in addition to diminished IL-6 and KC production in inflamed synovium. In conclusion, systemically delivered LV efficiently targets monocytes and macrophages in spleen that are involved in autoimmune arthritis. Moreover, this study confirms efficacy of TAK1 targeting in arthritis. This approach may provide a valuable tool in targeting splenic APCs, to unravel their role in autoimmune arthritis and to identify and validate APC specific therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2013

12. Enhanced suppressor of cytokine signaling 3 in arthritic cartilage dysregulates human chondrocyte function.

Author

Van De Loo, Fons A. J., Veenbergen, Sharon, Van Den Brand, Ben, Bennink, Miranda B., Blaney-Davidson, Esmeralda, Arntz, Onno J., Van Beuningen, Henk M., Van Der Kraan, Peter M., and Van Den Berg, Wim B.

Subjects

*CARTILAGE cells, *CELLULAR signal transduction, *CYTOKINES, *IMMUNOHISTOCHEMISTRY, *OSTEOARTHRITIS, *POLYMERASE chain reaction, *RESEARCH funding, *RHEUMATOID arthritis, *U-statistics, *WESTERN immunoblotting, *EQUIPMENT & supplies, *REVERSE transcriptase polymerase chain reaction, *DATA analysis software, *PHYSIOLOGY

Abstract

Objective To determine the expression of suppressor of cytokine signaling 3 (SOCS-3) in human articular chondrocytes and its functional consequences. Methods Chondrocytes were isolated from the cartilage of patients with osteoarthritis (OA), patients with rheumatoid arthritis (RA), and trauma patients and from the healthy cartilage of patients with a femoral neck fracture. The human chondrocyte cell line G6 and primary bovine chondrocytes were used in validation experiments. SOCS-3 messenger RNA (mRNA) expression was measured by quantitative polymerase chain reaction, and SOCS-3 protein levels were determined by Western blotting and immunohistochemical analysis. To ascertain the role of SOCS-3 in the chondrocyte response to interleukin-1β (IL-1β) or lipopolysaccharide (LPS), the expression of SOCS3 was either reduced by small interfering RNA or enhanced by viral transduction. Results The expression of SOCS-3 mRNA (but not that of SOCS-1 mRNA) was significantly enhanced in chondrocytes obtained from OA cartilage (mean ± SD ΔCt 3.4 ± 1.0) and RA cartilage (ΔCt 3.4 ± 1.4) compared with cartilage obtained from patients with femoral neck fracture (ΔCt 5.3 ± 1.2). The expression of SOCS3 correlated significantly with that of other genes known to be expressed in arthritic chondrocytes, such as MMP13 (r = 0.743), ADAMTS4 (r = 0.779), and ADAMTS5 (r = 0.647), and an inverse relationship was observed with COL2A1 (r = −0.561). Up-regulation of SOCS-3 by IL-1 in G6 chondrocytes and its spontaneous expression in OA chondrocytes were reduced by mithramycin, a specific inhibitor of transcription factor Sp-1. Overexpression of SOCS-3 in bovine chondrocytes reduced IL-1- and LPS-induced nitric oxide production and insulin-like growth factor 1-induced proteoglycan synthesis. Interestingly, a similar impairment of function was observed in OA chondrocytes, which was partially restored by SOCS-3 gene knockdown. Conclusion This study demonstrated that both SOCS-3 mRNA and SOCS-3 protein are expressed in human arthritic chondrocytes and affect cellular responses involved in cartilage pathology. [ABSTRACT FROM AUTHOR]

Published

2012

13. Splenic Suppressor of Cytokine Signaling 3 Transgene Expression Affects T Cell Responses and Prevents Development of Collagen-Induced Arthritis.

Author

Veenbergen, Sharon, Bennink, Miranda B., de Hooge, Alfons S. K., Arntz, Onno J., Smeets, Ruben L., van den Berg, Wim B., and van de Loo, Fons A. J.

Subjects

T cells, CELLULAR immunity, ARTHRITIS, CYTOKINES, COLLAGEN

Abstract

The article reports on the investigation of the modulation of T cell immunity for the treatment of experimental arthritis through enhanced expression of the suppressor of cytokine signaling in splenic antigen-presenting cells. The mice were immunized with collagen and adenovirus vectors were administered before the onset of collagen-induced arthritis.

Published

2008

14. Role of gene therapy in tissue engineering procedures in rheumatology: the use of animal models

Author

van der Kraan, Peter M., van de Loo, Fons A.J., and van den Berg, Wim B.

Subjects

*TISSUE engineering, *IMMUNODEFICIENCY, *SOMATOMEDIN, *ARTHRITIS

Abstract

Tissue engineering is not only the application of cells and scaffolds to generate a new tissue but should also bring into play biological principles to guide cellular behavior. A way to modify cellular behavior is genetic modification of the cells used for tissue engineering (gene therapy). In the field of rheumatic diseases, cellular modification by overexpressing anabolic factors, such as insulin-like growth factor-I or transforming growth factor β, or inhibitors of catabolic cytokines or proteolytic enzymes can protect tissues form further destruction and stimulate tissue repair. To test the effect of transgenes on tissue engineering adequate test systems have to be available. Initial testing can be done in simple in vitro systems. However, animal models are unavoidable to study the interaction between the environment and tissue engineering. Optimal models to study gene therapy in combination with tissue engineering in the field of rheumatology are not available at this moment. Arthritis models are mainly developed in small animals while high-quality tissue engineering experiments ask for a large animal model. Development of animal models that can be used for tissue engineering experiments and mimic end stage arthritic diseases is needed. [Copyright &y& Elsevier]

Published

2004