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4. The role of Th17 cells in juvenile idiopathic arthritis

Author

Nistala, K.

Subjects
616.7
Abstract

Autoimmune arthritis in childhood, know as juvenile idiopathic arthritis (JIA), has a heterogeneity, ranging from monoarthritis to recalcitrant polyarthritis, making it a model disease in which to study immuno-regulation. Regulatory T cells, key players in peripheral immune homeostasis are enriched in the joints of JIA patients, particularly those with mild arthritis. To test the factors that lead to this enrichment, Treg trafficking was examined in the context of JIA. Synovial Treg showed enhanced chemotaxis to the inflammatory chemokine CCL5, widely detectable within the joint, when compared to Treg from peripheral blood. The trafficking of a related, but highly inflammatory T cell subset, Th17 cells, was also investigated. Th17 cells play a dominant role in murine models of arthritis, yet their contribution to human disease is unknown. The data presented here, showed that IL-17+ CD4 T cells were enriched in the joints of JIA patients, by a CCR6 dependent mechanism and importantly, their frequency correlated with the severity of disease course. The majority of synovial IL-17+ CD4 T cells expressed a cytokine and chemokine receptor phenotype intermediate between Th17 and Th1. Here it was shown that these cells (Th17/1) expressed high levels of both Th17 and Th1 specific transcription factors, RORC2 and T-bet. Modelling the generation of Th17/1 in vitro, Th17 cells ‘converted’ to Th17/1 under conditions which mimicked the disease site, namely low TGFβ and high IL-12 levels. Using CD161, a human Th17 marker, it was shown that synovial Th17/1 cells, and unexpectedly, a large proportion of Th1 cells expressed CD161. This study provided evidence to support a Th17 origin for Th1 cells expressing CD161. In vitro, Th17 cells which converted to a Th1 phenotype maintained CD161 expression, whilst in the joint CD161+ Th1 cells shared features with Th17 cells, with shared T cell receptor clonality and expression of RORC2, although they were IL-17 negative. We propose that Th17 cells may 'convert' to Th17/1 and Th1 cells in human arthritis. Therefore therapies targeting the induction of Th17 cells could also attenuate the Th17/1 and Th1 effector populations within the inflamed joint.

Published
2011

11. Galectin-9 and CXCL10 as Biomarkers for Disease Activity in Juvenile Dermatomyositis: A Longitudinal Cohort Study and Multicohort Validation

Author

Wienke, J., Enders, F.B., Lim, J, Mertens, J.S., van den Hoogen, L. L., Wijngaarde, C.A., Yeo, J.G., Meyer, A. (Andreas), Otten, H.G. (Henderikus), Fritsch-Stork, R. D. E., Kamphuis, S.S.M. (Sylvia), Hoppenreijs, E., Armbrust, W. (Wineke), van den Berg, J.M., Muller, P., Tekstra, J., Hoogendijk, J.E., Deakin, C.T., Jager, W. (Wilco) de, Roon, J.A.G. (J. A G) van, Pol, W.-L. (W-Ludo) van der, Nistala, K., Pilkington, C., Visser, M. (Mirjam), Arkachaisri, T., Radstake, T, Kooj, A.J. (Anneke), Nierkens, S., Wedderburn, L.R. (Lucy), van Royen-kerkhof, A., van Wijk, F., Wienke, J., Enders, F.B., Lim, J, Mertens, J.S., van den Hoogen, L. L., Wijngaarde, C.A., Yeo, J.G., Meyer, A. (Andreas), Otten, H.G. (Henderikus), Fritsch-Stork, R. D. E., Kamphuis, S.S.M. (Sylvia), Hoppenreijs, E., Armbrust, W. (Wineke), van den Berg, J.M., Muller, P., Tekstra, J., Hoogendijk, J.E., Deakin, C.T., Jager, W. (Wilco) de, Roon, J.A.G. (J. A G) van, Pol, W.-L. (W-Ludo) van der, Nistala, K., Pilkington, C., Visser, M. (Mirjam), Arkachaisri, T., Radstake, T, Kooj, A.J. (Anneke), Nierkens, S., Wedderburn, L.R. (Lucy), van Royen-kerkhof, A., and van Wijk, F.

Abstract

Objective. Objective evaluation of disease activity is challenging in patients with juvenile dermatomyositis (DM) due to a lack of reliable biomarkers, but it is crucial to avoid both under- and overtreatment of patients. Recently, we identified 2 proteins, galectin-9 and CXCL10, whose levels are highly correlated with the extent of juvenile DM disease activity. This study was undertaken to validate galectin-9 and CXCL10 as biomarkers for disease activity in juvenile DM, and to assess their disease specificity and potency in predicting the occurrence of flares. Methods. Levels of galectin-9 and CXCL10 were measured by multiplex immunoassay in serum samples from 125 unique patients with juvenile DM in 3 international cross-sectional cohorts and a local longitudinal cohort. The disease specificity of both proteins was examined in 50 adult patients with DM or nonspecific myositis (NSM) and 61 patients with other systemic autoimmune diseases. Results. Both cross-sectionally and longitudinally, galectin-9 and CXCL10 outperformed the currently used laboratory marker, creatine kinase (CK), in distinguishing between juvenile DM patients with active disease and those in remission (area under the receiver operating characteristic curve [AUC] 0.86–0.90 for galectin-9 and CXCL10; AUC 0.66–0.68 for CK). The sensitivity and specificity for active disease in juvenile DM was 0.84 and 0.92, respectively, for galectin-9 and 0.87 and 1.00, respectively, for CXCL10. In 10 patients with juvenile DM who experienced a flare and were prospectively followed up, continuously elevated or rising biomarker levels suggested an imminent flare up to several months before the onset of symptoms, even in the absence of elevated CK levels. Galectin-9 and CXCL10 distinguished between active disease and remission in adult patients with DM or NSM (P = 0.0126 for galectin-9 and P < 0.0001 for CXCL10) and were suited for measurement in minimally invasive dried blood spots (healthy controls versus juvenile

Published
2019
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12. Galectin-9 and CXCL10 as Biomarkers for Disease Activity in Juvenile Dermatomyositis: A Longitudinal Cohort Study and Multicohort Validation

Author

Wienke, J, Enders, FB, Lim, J, Mertens, JS, van den Hoogen, L L, Wijngaarde, CA, Yeo, JG, Meyer, A, Otten, HG, Fritsch-Stork, R D E, Kamphuis, Sylvia, Hoppenreijs, E, Armbrust, W, Berg, JM, Muller, P, Tekstra, J, Hoogendijk, JE, Deakin, CT, de Jager, W, van Roon, JAG, van der Pol, WL, Nistala, K, Pilkington, C, Visser, M, Arkachaisri, T, Radstake, T, van der Kooi, AJ, Nierkens, S, Wedderburn, LR, van Royen-kerkhof, A, van Wijk, F, Wienke, J, Enders, FB, Lim, J, Mertens, JS, van den Hoogen, L L, Wijngaarde, CA, Yeo, JG, Meyer, A, Otten, HG, Fritsch-Stork, R D E, Kamphuis, Sylvia, Hoppenreijs, E, Armbrust, W, Berg, JM, Muller, P, Tekstra, J, Hoogendijk, JE, Deakin, CT, de Jager, W, van Roon, JAG, van der Pol, WL, Nistala, K, Pilkington, C, Visser, M, Arkachaisri, T, Radstake, T, van der Kooi, AJ, Nierkens, S, Wedderburn, LR, van Royen-kerkhof, A, and van Wijk, F

Published
2019

17. Early changes in gene expression and inflammatory proteins in systemic juvenile idiopathic arthritis patients on canakinumab therapy

Author

Brachat A. H., Grom A. A., Wulffraat N., Brunner H. I., Quartier P., Brik R., McCann L., Ozdogan H., Rutkowska-Sak L., Schneider R., Gerloni V., Harel L., Terreri M., Houghton K., Joos R., Kingsbury D., Lopez-Benitez J. M., Bek S., Schumacher M., Valentin M. -A., Gram H., Abrams K., Martini A., Lovell D. J., Nirmala N. R., Ruperto N., Cuttica R., Emminger W., Lauwerys B., Wouters C., Goffin L., Sztajnbok F., Radominski S., Oliveira S., Haddad E., Kone-Paut I., Desjonqueres M., Fischbach M., Thon A., Foell D., Weibarth-Riedel E., Horneff G., Trauzeddel R., Berner R., Kallinich T., Trachana M., Constantin T., Barash J., Berkun Y., Uziel Y., Corona F., Alessio M., Cimaz R., Viola S., Flato B., Ferrandiz M., Calvo I., Anton J., Robledillos J. C., Gamir M. L., Magnusson B., Hofer M., Unsal E., Erguven M., Ozen S., Wilkinson N., Chieng A., Ramanan A., Foster H., Nistala K., Higgins G., Marzan K., Schikler K., Morris P., Brachat, A. H., Grom, A. A., Wulffraat, N., Brunner, H. I., Quartier, P., Brik, R., Mccann, L., Ozdogan, H., Rutkowska-Sak, L., Schneider, R., Gerloni, V., Harel, L., Terreri, M., Houghton, K., Joos, R., Kingsbury, D., Lopez-Benitez, J. M., Bek, S., Schumacher, M., Valentin, M. -A., Gram, H., Abrams, K., Martini, A., Lovell, D. J., Nirmala, N. R., Ruperto, N., Cuttica, R., Emminger, W., Lauwerys, B., Wouters, C., Goffin, L., Sztajnbok, F., Radominski, S., Oliveira, S., Haddad, E., Kone-Paut, I., Desjonqueres, M., Fischbach, M., Thon, A., Foell, D., Weibarth-Riedel, E., Horneff, G., Trauzeddel, R., Berner, R., Kallinich, T., Trachana, M., Constantin, T., Barash, J., Berkun, Y., Uziel, Y., Corona, F., Alessio, M., Cimaz, R., Viola, S., Flato, B., Ferrandiz, M., Calvo, I., Anton, J., Robledillos, J. C., Gamir, M. L., Magnusson, B., Hofer, M., Unsal, E., Erguven, M., Ozen, S., Wilkinson, N., Chieng, A., Ramanan, A., Foster, H., Nistala, K., Higgins, G., Marzan, K., Schikler, K., and Morris, P.

Subjects
Male, 0301 basic medicine, SJIA, Juvenile, Arthritis, 0302 clinical medicine, Monoclonal, Gene expression, Child, Oligonucleotide Array Sequence Analysis, Immunoassay, biology, Interleukin-18, Antibodies, Monoclonal, Interleukin-1β, Child, Preschool, Female, Interleukin 18, Biomarkers, Canakinumab, Juvenile idiopathic arthritis, Adolescent, Arthritis, Juvenile, Down-Regulation, Gene Expression Profiling, Humans, Interleukin-6, Transcriptome, Young Adult, Research Article, Human, medicine.drug, medicine.medical_specialty, Antibodies, Monoclonal, Humanized, Antibodies, 03 medical and health sciences, Juvenile idiopathic arthriti, Internal medicine, medicine, Journal Article, Preschool, Interleukin 6, 030203 arthritis & rheumatology, Oligonucleotide Array Sequence Analysi, business.industry, Microarray analysis techniques, Interleukin-1 beta, Biomarker, medicine.disease, Rheumatology, Gene expression profiling, 030104 developmental biology, Immunology, biology.protein, business
Abstract

Novartis Pharma Background: Canakinumab is a human anti-interleukin-1 beta (IL-1 beta) monoclonal antibody neutralizing IL-1 beta-mediated pathways. We sought to characterize the molecular response to canakinumab and evaluate potential markers of response using samples from two pivotal trials in systemic juvenile idiopathic arthritis (SJIA). Methods: Gene expression was measured in patients with febrile SJIA and in matched healthy controls by Affymetrix DNA microarrays. Transcriptional response was assessed by gene expression changes from baseline to day 3 using adapted JIA American College of Rheumatology (aACR) response criteria (50 aACR JIA). Changes in pro-inflammatory cytokines IL-6 and IL-18 were assessed up to day 197. Results: Microarray analysis identified 984 probe sets differentially expressed (>= 2-fold difference P < 0.05) in patients versus controls. Over 50% of patients with >= 50 aACR JIA were recognizable by baseline expression values. Analysis of gene expression profiles from patients achieving = 50 aACR JIA response at day 15 identified 102 probe sets differentially expressed upon treatment (>= 2-fold difference P < 0.05) on day 3 versus baseline, including IL-1 beta, IL-1 receptors (IL1-R1 and IL1-R2), IL-1 receptor accessory protein (IL1-RAP), and IL-6. The strongest clinical response was observed in patients with higher baseline expression of dysregulated genes and a strong transcriptional response on day 3. IL-6 declined by day 3 (>= 8-fold decline P < 0.0001) and remained suppressed. IL-18 declined on day 57 (>= 1.5-fold decline, P

Published
2017

19. Consensus-based recommendations for the management of juvenile dermatomyositis

Author

Enders, F.B., Bader-Meunier, B., Baildam, E., Constantin, T., Dolezalova, P., Feldman, B.M., Lahdenne, P., Magnusson, B., Nistala, K., Ozen, S., Pilkington, C., Ravelli, A., Russo, R., Uziel, Y., van Brussel, M., van der Net, J., Vastert, S., Wedderburn, L.R., Wulffraat, N., McCann, L.J., and van Royen-Kerkhof, A.

Abstract

In 2012, a European initiative called Single Hub and Access point for pediatric Rheumatology in Europe (SHARE) was launched to optimise and disseminate diagnostic and management regimens in Europe for children and young adults with rheumatic diseases. Juvenile dermatomyositis (JDM) is a rare disease within the group of paediatric rheumatic diseases (PRDs) and can lead to significant morbidity. Evidence-based guidelines are sparse and management is mostly based on physicians' experience. Consequently, treatment regimens differ throughout Europe. To provide recommendations for diagnosis and treatment of JDM. Recommendations were developed by an evidence-informed consensus process using the European League Against Rheumatism standard operating procedures. A committee was constituted, consisting of 19 experienced paediatric rheumatologists and 2 experts in paediatric exercise physiology and physical therapy, mainly from Europe. Recommendations derived from a validated systematic literature review were evaluated by an online survey and subsequently discussed at two consensus meetings using nominal group technique. Recommendations were accepted if >80% agreement was reached. In total, 7 overarching principles, 33 recommendations on diagnosis and 19 recommendations on therapy were accepted with >80% agreement among experts. Topics covered include assessment of skin, muscle and major organ involvement and suggested treatment pathways. The SHARE initiative aims to identify best practices for treatment of patients suffering from PRD. Within this remit, recommendations for the diagnosis and treatment of JDM have been formulated by an evidence-informed consensus process to produce a standard of care for patients with JDM throughout Europe.

Published
2017

21. Single Hub and Access Point for Paediatric Rheumatology in Europe (SHARE)- Evidence Based Recommendations for Diagnosis and Treatment of Juvenile Idiopathic Arthritis

Author

Vastert, S. J., Boom, Victor, Anton, Jordi, Constantin, Tamas, Pavla Doležalová, Horneff, Gerd, Lahdenne, Pekka, Magnusson, Bo, Minden, Kirsten, Nistala, K., Quartier, Pierre, Rumba-Rozenfelde, Ingrida, Ruperto, Nicolino, Piccolo, Vanessa Remy, Russo, Ricardo A. G., Uziel, Yosef, Wouters, Carine, Martini, Alberto, Ravelli, Angelo, Foster, Helen, and Wulffraat, Nico

Published
2014

22. Delineation of the Innate and Adaptive T-Cell Immune Outcome in the Human Host in Response to Campylobacter jejuni Infection

Author

Edwards, L. A., Nistala, K., Mills, D. C., Stephenson, H. N., Zilbauer, M., Wren, B. W., Dorrell, N., Lindley, K. J., Wedderburn, L. R., and Bajaj-Elliott, M.

Subjects
INFLAMMATORY-BOWEL-DISEASE, NATURAL-KILLER-CELLS, DENDRITIC CELLS, CYTOKINE PRODUCTION, INTESTINAL-MUCOSA, ESCHERICHIA-COLI, INTERLEUKIN 22, IN-VITRO, PATHOGENESIS, BETA-DEFENSIN-2
Abstract

Background: Campylobacter jejuni is the most prevalent cause of bacterial gastroenteritis worldwide. Despite the significant health burden this infection presents, molecular understanding of C. jejuni-mediated disease pathogenesis remains poorly defined. Here, we report the characterisation of the early, innate immune response to C. jejuni using an ex-vivo human gut model of infection. Secondly, impact of bacterial-driven dendritic cell activation on T-cell mediated immunity was also sought.Methodology: Healthy, control paediatric terminal ileum or colonic biopsy tissue was infected with C. jejuni for 8-12 hours. Bacterial colonisation was followed by confocal microscopy and mucosal innate immune responses measured by ELISA. Marked induction of IFN gamma with modest increase in IL-22 and IL-17A was noted. Increased mucosal IL-12, IL-23, IL-1 beta and IL-6 were indicative of a cytokine milieu that may modulate subsequent T-cell mediated immunity. C. jejuni-driven human monocyte-derived dendritic cell activation was followed by analyses of T cell immune responses utilising flow cytometry and ELISA. Significant increase in Th-17, Th-1 and Th-17/Th-1 double-positive cells and corresponding cytokines was observed. The ability of IFN gamma, IL-22 and IL-17 cytokines to exert host defence via modulation of C. jejuni adhesion and invasion to intestinal epithelia was measured by standard gentamicin protection assay.Conclusions: Both innate and adaptive T cell-immunity to C. jejuni infection led to the release of IFN gamma, IL-22 and IL-17A; suggesting a critical role for this cytokine triad in establishing host anti-microbial immunity during the acute and effectors phase of infection. In addition, to their known anti-microbial functions; IL-17A and IL-17F reduced the number of intracellular C. jejuni in intestinal epithelia, highlighting a novel aspect of how IL-17 family members may contribute to protective immunity against C. jejuni.

Published
2010

24. OP0150 Development and Preliminary Validation of a New Composite Disease Activity Measure for Juvenile Dermatomyositis

Author

Consolaro, A., primary, Varnier, G.C., additional, Ferrari, C., additional, de Inocencio, J., additional, Civino, A., additional, Jeluzic-Drazic, M., additional, Tsitsamis, E., additional, Vojinovic, J., additional, Makay, B., additional, Espada, G., additional, Malattia, C., additional, Maillard, S., additional, Martini, A., additional, Pilkington, C., additional, Ravelli, A., additional, and Nistala, K., additional

Published
2015
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25. Effective induction therapy for anti-SRP associated myositis in childhood: A small case series and review of the literature.

Author

Binns, E. L., Moraitis, E., Maillard, S., Tansley, S., McHugh, N., Jacques, T. S., Wedderburn, L. R., Pilkington, C., Yasin, S. A., and Nistala, K.

Subjects
MYOSITIS, CYCLOPHOSPHAMIDE, METHOTREXATE, PHYSIOLOGICAL therapeutics, THERAPEUTICS
Abstract

Background: Anti-Signal Recognition Particle associated myopathy is a clinically and histopathologically distinct subgroup of Juvenile Idiopathic Inflammatory Myositis, which is under-recognised in children and fails to respond to conventional first line therapies. We present three cases where remission was successfully induced using combination therapy with intensive rehabilitation. Case presentations: Three new patients are reported. All 3 cases presented with profound, rapid-onset, proximal myopathy and markedly raised CK, but no rash. Histology revealed a destructive myopathy characterized by scattered atrophic and necrotic fibres with little or no inflammatory infiltrate. All 3 patients responded to induction with cyclophosphamide, IVIG and rituximab, in conjunction with intensive physiotherapy and methotrexate as the maintenance agent. Our patients regained near-normal strength (MMT > 70/80), in contrast with the current literature where >50% of cases reported severe residual weakness. A literature search on paediatric anti-SRP myositis was performed to June 2016; PubMed was screened using a combination of the following terms: signal recognition particle, autoantibodies, antibodies, myositis, muscular diseases, skeletal muscle, childhood, paediatric, juvenile. Articles in a foreign language were excluded. Nine case studies were found. Conclusion: This paper supports the hypothesis that anti-SRP myositis is distinct from other JIIM. It is an important differential to JDM and should be considered where there is severe weakness without rash or if highly elevated muscle enzymes (CK > 10,000 U/l) are found. Early identification is essential to initiate aggressive medical and physical therapy. Greater international collaboration and long-term follow-up data is needed to establish the most effective treatment strategy for this rare group of patients. [ABSTRACT FROM AUTHOR]

Published
2017
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26. Canakinumab treatment shows maintained efficacy in systemic juvenile idiopathic arthritis patients

Author

Wulffraat, NM, primary, Ruperto, N, additional, Brunner, HI, additional, Oliveira, S, additional, Uziel, Y, additional, Nistala, K, additional, Cimaz, R, additional, Ferrandiz, MA, additional, Flato, B, additional, Gamir, M, additional, Kone-Paut, I, additional, Gaillez, C, additional, Lheritier, K, additional, Abrams, K, additional, Martini, A, additional, and Lovell, D, additional

Published
2014
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27. OP0180 Maintenance of Efficacy by Canakinumab Treatment in Systemic Juvenile Idiopathic Arthritis Patients

Author

Wulffraat, N.M., primary, Ruperto, N., additional, Brunner, H.I., additional, Oliveira, S., additional, Uziel, Y., additional, Nistala, K., additional, Cimaz, R., additional, Ferrandiz, M.A., additional, Flato, B., additional, Gamir, M.L., additional, Koné-Paut, I., additional, Gaillez, C., additional, Lheritier, K., additional, Abrams, K., additional, Martini, A., additional, and Lovell, D.J., additional

Published
2014
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29. AB1182 Efficacy and safety of canakinumab, fully human anti-interleukin-1beta antibody, in systemic juvenile idiopathic arthritis

Author

Ruperto, N., primary, Brunner, H., additional, Quartier, P., additional, Constantin, T., additional, Wulffraat, N., additional, Horneff, G., additional, Brik, R., additional, McCann, L., additional, Kasapcopur, O., additional, Rutkowska-Sak, L., additional, Schneider, R., additional, Berkun, Y., additional, Calvo, I., additional, Erguven, M., additional, Goffin, L., additional, Hofer, M., additional, Kallinich, T., additional, Knupp, S., additional, Uziel, Y., additional, Viola, S., additional, Nistala, K., additional, Wouters, C., additional, Cimaz, R., additional, Ferrandiz, M., additional, Flato, B., additional, Luz Gamir, M., additional, Kone-Paut, I., additional, Grom, A., additional, Magnusson, B., additional, Ozen, S., additional, Sztajnbok, F., additional, Lheritier, K., additional, Kim, D., additional, Abrams, K., additional, Martini, A., additional, and Lovell, D., additional

Published
2013
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33. The role of muscle ultrasound in juvenile dermatomyositis (JDM)

Author

Nistala, K., Owens, C., de Bruyn, R., and Pilkington, C.

Subjects
Children -- Health aspects -- Research, Dermatomyositis -- Care and treatment -- Research, Family and marriage, Health, Care and treatment, Research, Health aspects
Abstract

Background: Optimum treatment in JDM requires an accurate, validated assessment tool to identify remission or relapse. Current methods used for assessing disease activity have limitations. Our aim was to test [...]

Published
2004

34. Co-existent sickle cell disease and juvenile rheumatoid arthritis. Two cases with delayed diagnosis and severe destructive arthropathy.

Author

Nistala, K and Murray, K J

Abstract

We describe 2 pediatric patients with sickle cell disease (SCD) who developed seropositive juvenile rheumatoid arthritis (JRA). Both patients have severe joint damage, the compound effect of both disease processes. The bone and cartilage destruction, which poses serious therapeutic challenges, highlights the difficulty of making a diagnosis of chronic inflammatory disease in the setting of SCD. There may be a correlation between increased levels of tumor necrosis factor-alpha in the synovial tissue of joints damaged by arthritis and local sickling. The resultant ischemia and corresponding inflammatory infiltrates could in turn worsen existing synovial proliferation and cartilage destruction as well as trigger further sickling.

Published
2001

36. Efficacy, safety and tolerability of GSK3858279, an anti-CCL17 monoclonal antibody and analgesic, in healthy volunteers and patients with knee osteoarthritis pain: a phase I, randomised, double-blind, placebo-controlled, proof-of-mechanism and proof-of-concept study.

Author

Nijjar JS, Abbott-Banner K, Alvarez Y, Aston N, Bass D, Bentley JH, Ellis J, Ellson C, Emery EC, Feeney M, Fernando D, Inman D, Kaur R, Modis LK, Munoz Vicente S, Muya C, Nistala K, Panoilia E, Ray R, Siederer S, Smith JE, Weir L, and Wisniacki N

Abstract

Objectives: The objective of this study was to evaluate efficacy, safety and tolerability of the first-in-class, anti-CCL17 monoclonal antibody, GSK3858279, in treating knee osteoarthritis (OA) pain., Methods: This was a phase I, randomised, placebo-controlled, two-part, proof-of-mechanism and proof-of-concept study. In part A, healthy participants were randomised 3:1 to receive GSK3858279 as either single intravenous (0.1-10 mg/kg) doses, a subcutaneous (3 mg/kg up to 240 mg maximum) dose, or placebo, to evaluate safety and tolerability. In part B, participants with knee OA pain were randomised 1:1 to receive weekly subcutaneous 240 mg GSK3858279, or placebo, for 8 weeks, to assess safety and change from baseline (CFB) in average and worst knee pain intensity. Exploratory endpoints included CFB in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) pain, function and stiffness scores., Results: GSK3858279 demonstrated greater median CFB (95% credible interval (CrI)) in average and worst knee pain intensity versus placebo (average, -1.18 (-2.15, -0.20); worst, -1.09 (-2.29, 0.12)) at week 8. Median CFB (95% CrI) for GSK3858279 versus placebo in WOMAC pain and function scores were -1.41 (-2.35, -0.46) and -1.29 (-2.28, -0.29), respectively, at week 8. Overall, 72% (26/36; part A) and 88% (21/24; part B) of participants receiving GSK3858279 experienced adverse events (AEs); with nasopharyngitis being the most common in part A and injection site reactions in part B. No serious AEs or deaths were observed.GSK3858279 improved pain intensity and WOMAC pain and function scores in adults with knee OA pain and demonstrated favourable safety and tolerability in both healthy participants and adults with knee OA pain., Competing Interests: Competing interests: JSN, JE, KA-B, RR, SMV, JHB, CM, SS, EP, YA, DB, DF, RK, DI, CE, MF, JES, LW and NW are employed by GSK and hold financial equities in GSK. NA was employed by GSK and held financial equities in GSK at the time of study conduct. ECE was employed by GSK and held financial equities in GSK at the time of the study conduct; and is currently employed by, and holds shares in, AstraZeneca. LKM was employed by GSK and held financial equities in GSK at the time of study conduct; and is currently employed by, and holds shares in, Amphista Therapeutics. KN was employed by GSK and held financial equities in GSK at the time of study conduct and was a previous employee of and shareholder in AstraZeneca., (© Author(s) (or their employer(s)) 2024. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ on behalf of EULAR.)

Published
2024
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37. Immune complex disease in a chronic monkey study with a humanised, therapeutic antibody against CCL20 is associated with complement-containing drug aggregates.

Author

Laffan SB, Thomson AS, Mai S, Fishman C, Kambara T, Nistala K, Raymond JT, Chen S, Ramani T, Pageon L, Polsky R, Watkins M, Ottolangui G, White JR, Maier C, Herdman M, and Bouma G

Subjects
Animals, Antibodies, Monoclonal toxicity, Chronic Disease, Crystallization, Endpoint Determination, Female, Humans, Inflammation immunology, Inflammation pathology, Macaca fascicularis, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal, Humanized therapeutic use, Chemokine CCL20 immunology, Complement System Proteins immunology, Immune Complex Diseases drug therapy, Immune Complex Diseases immunology, Immunoconjugates therapeutic use
Abstract

Despite the potential for the chemokine class as therapeutic targets in immune mediated disease, success has been limited. Many chemokines can bind to multiple receptors and many receptors have multiple ligands, with few exceptions. One of those exceptions is CCL20, which exclusively pairs to CCR6 and is associated with several immunologic conditions, thus providing a promising therapeutic target. Following successful evaluation in a single dose, first time in human clinical study, GSK3050002-a humanized IgG1 monoclonal antibody against human CCL20-was evaluated in a 26-week cynomolgus monkey toxicology study. A high incidence of unexpected vascular and organ inflammation was observed microscopically, leading to the decision to halt clinical development. Here we report a dose-responsive increase in the incidence and severity of inflammation in multiple organs from monkeys receiving 30 and 300 mg/kg/week by either subcutaneous or intravenous injection. Histomorphological changes resembled an immune complex-mediated pathology, which is often due to formation of anti-drug antibodies in monkeys receiving a human protein therapeutic and thus not predictive of clinical outcome. However, the presentation was atypical in that there was a clear dose response with a very high incidence of inflammation with a low incidence of ADA that did not correlate well individually. Additionally, the immunohistologic presentation was atypical in that the severity and distribution of tissue inflammation was greater than the numbers of associated immune complexes (i.e., granular deposits). An extensive ex vivo analysis of large molecular weight protein complexes in monkey serum from this study and in human serum samples demonstrated a time-dependent aggregation of GSK3050002, that was not predicted by in vitro assays. The aggregates also contained complement components. These findings support the hypothesis that immune complexes of drug aggregates, not necessarily including anti-drug antibodies, can fix complement, accumulate over time, and trigger immune complex disease. A situation which may have increased clinical relevance than typical anti-drug antibody-associated immune complex disease in monkeys administered human antibody proteins., Competing Interests: Funding for this study was provided by GlaxoSmithKline and Morphotek, Inc. (NCT01984047). JR is an employee of Charles River Laboratories and principal investigator of the immunohistochemistry analysis. TR is an employee of Covance CRS, LLC (formerly Envigo CRS) and study director of the 26-week monkey toxicity study. LP was an employee of Envigo CRS for the duration of the study. All other listed authors were employees of GlaxoSmithKline (GSK) during the conduct of the study, hold GSK stock or stock options, and meet the criteria for authorship set forth by the International Committee for Medical Journal Editors. This does not alter our adherence to PLOS ONE policies on sharing data and materials.

Published
2020
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38. Aryl Hydrocarbon Receptor Contributes to the Transcriptional Program of IL-10-Producing Regulatory B Cells.

Author

Piper CJM, Rosser EC, Oleinika K, Nistala K, Krausgruber T, Rendeiro AF, Banos A, Drozdov I, Villa M, Thomson S, Xanthou G, Bock C, Stockinger B, and Mauri C

Subjects
Animals, Antigens, CD genetics, Antigens, CD immunology, B-Lymphocytes, Regulatory cytology, Basic Helix-Loop-Helix Transcription Factors genetics, Cell Differentiation genetics, Interleukin-10 genetics, Mice, Mice, Knockout, Receptors, Aryl Hydrocarbon genetics, Th1 Cells cytology, Th1 Cells immunology, Th17 Cells cytology, Th17 Cells immunology, B-Lymphocytes, Regulatory immunology, Basic Helix-Loop-Helix Transcription Factors immunology, Cell Differentiation immunology, Interleukin-10 immunology, Receptors, Aryl Hydrocarbon immunology, Transcription, Genetic immunology
Abstract

Regulatory B cells (Bregs) play a critical role in the control of autoimmunity and inflammation. IL-10 production is the hallmark for the identification of Bregs. However, the molecular determinants that regulate the transcription of IL-10 and control the Breg developmental program remain unknown. Here, we demonstrate that aryl hydrocarbon receptor (AhR) regulates the differentiation and function of IL-10-producing CD19 + CD21 hi CD24 hi Bregs and limits their differentiation into B cells that contribute to inflammation. Chromatin profiling and transcriptome analyses show that loss of AhR in B cells reduces expression of IL-10 by skewing the differentiation of CD19 + CD21 hi CD24 hi B cells into a pro-inflammatory program, under Breg-inducing conditions. B cell AhR-deficient mice develop exacerbated arthritis, show significant reductions in IL-10-producing Bregs and regulatory T cells, and show an increase in T helper (Th) 1 and Th17 cells compared with B cell AhR-sufficient mice. Thus, we identify AhR as a relevant contributor to the transcriptional regulation of Breg differentiation., (Copyright © 2019 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published
2019
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39. Galectin-9 and CXCL10 as Biomarkers for Disease Activity in Juvenile Dermatomyositis: A Longitudinal Cohort Study and Multicohort Validation.

Author

Wienke J, Bellutti Enders F, Lim J, Mertens JS, van den Hoogen LL, Wijngaarde CA, Yeo JG, Meyer A, Otten HG, Fritsch-Stork RDE, Kamphuis SSM, Hoppenreijs EPAH, Armbrust W, van den Berg JM, Hissink Muller PCE, Tekstra J, Hoogendijk JE, Deakin CT, de Jager W, van Roon JAG, van der Pol WL, Nistala K, Pilkington C, de Visser M, Arkachaisri T, Radstake TRDJ, van der Kooi AJ, Nierkens S, Wedderburn LR, van Royen-Kerkhof A, and van Wijk F

Subjects
Adolescent, Adult, Biomarkers blood, Child, Creatine Kinase blood, Cross-Sectional Studies, Female, Follow-Up Studies, Humans, Longitudinal Studies, Male, Predictive Value of Tests, Prospective Studies, Reproducibility of Results, Sensitivity and Specificity, Young Adult, Chemokine CXCL10 blood, Dermatomyositis blood, Dermatomyositis diagnosis, Galectins blood, Severity of Illness Index
Abstract

Objective: Objective evaluation of disease activity is challenging in patients with juvenile dermatomyositis (DM) due to a lack of reliable biomarkers, but it is crucial to avoid both under- and overtreatment of patients. Recently, we identified 2 proteins, galectin-9 and CXCL10, whose levels are highly correlated with the extent of juvenile DM disease activity. This study was undertaken to validate galectin-9 and CXCL10 as biomarkers for disease activity in juvenile DM, and to assess their disease specificity and potency in predicting the occurrence of flares., Methods: Levels of galectin-9 and CXCL10 were measured by multiplex immunoassay in serum samples from 125 unique patients with juvenile DM in 3 international cross-sectional cohorts and a local longitudinal cohort. The disease specificity of both proteins was examined in 50 adult patients with DM or nonspecific myositis (NSM) and 61 patients with other systemic autoimmune diseases., Results: Both cross-sectionally and longitudinally, galectin-9 and CXCL10 outperformed the currently used laboratory marker, creatine kinase (CK), in distinguishing between juvenile DM patients with active disease and those in remission (area under the receiver operating characteristic curve [AUC] 0.86-0.90 for galectin-9 and CXCL10; AUC 0.66-0.68 for CK). The sensitivity and specificity for active disease in juvenile DM was 0.84 and 0.92, respectively, for galectin-9 and 0.87 and 1.00, respectively, for CXCL10. In 10 patients with juvenile DM who experienced a flare and were prospectively followed up, continuously elevated or rising biomarker levels suggested an imminent flare up to several months before the onset of symptoms, even in the absence of elevated CK levels. Galectin-9 and CXCL10 distinguished between active disease and remission in adult patients with DM or NSM (P = 0.0126 for galectin-9 and P < 0.0001 for CXCL10) and were suited for measurement in minimally invasive dried blood spots (healthy controls versus juvenile DM, P = 0.0040 for galectin-9 and P < 0.0001 for CXCL10)., Conclusion: In this study, galectin-9 and CXCL10 were validated as sensitive and reliable biomarkers for disease activity in juvenile DM. Implementation of these biomarkers into clinical practice as tools to monitor disease activity and guide treatment might facilitate personalized treatment strategies., (© 2019 The Authors. Arthritis & Rheumatology published by Wiley Periodicals, Inc. on behalf of American College of Rheumatology.)

Published
2019
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40. Development and validation of a composite disease activity score for measurement of muscle and skin involvement in juvenile dermatomyositis.

Author

Rosina S, Consolaro A, van Dijkhuizen P, Pistorio A, Varnier GC, Bovis F, Nistala K, Maillard S, Civino A, Tsitsami E, de Inocencio J, Jelusic M, Vojinovic J, Espada G, Makay B, Katsicas MM, Pratsidou-Gertsi P, Lazarevic D, Rao AP, Pires Marafon D, Martini A, Pilkington C, Ruperto N, and Ravelli A

Subjects
Attitude to Health, Child, Child, Preschool, Dermatomyositis physiopathology, Dermatomyositis therapy, Factor Analysis, Statistical, Female, Humans, Male, Muscle Strength, Outcome Assessment, Health Care methods, Parents psychology, Quality of Life, Reproducibility of Results, Dermatomyositis diagnosis, Severity of Illness Index
Abstract

Objective: To develop a composite DAS for JDM and provide preliminary evidence of its validity., Methods: The Juvenile DermatoMyositis Activity Index (JDMAI) is composed of four items: physician's global assessment of overall disease activity; parent's/child's global assessment of child's wellbeing; measurement of muscle strength; and assessment of skin disease activity. The score of the JDMAI is the arithmetic sum of the scores of each individual component. Six versions of the JDMAI were tested, which differed in the tools used to assess the third and fourth items. Validation procedures were conducted using three large multinational patient samples including a total of 627 patients., Results: The JDMAI was found to possess face and content validity, good construct validity, satisfactory internal consistency (Cronbach's alpha = 0.58-0.89), fair responsiveness to clinically important change (standardized response mean = 0.82-3.12 among patients improved) and strong capacity to discriminate patients judged as being in the state of inactive disease or low, moderate or high disease activity by the physician (P < 0.001) or whose parents were satisfied or not satisfied with the course of their child's illness (P < 0.001). Overall, the six versions of the JDMAI showed similar metrological performances in validation analyses., Conclusion: The JDMAI was found to possess good measurement properties in a large population of patients with a wide range of disease activity, and is, therefore, suitable for use in both clinical and research settings. The final version of the JDMAI will be selected after its prospective validation., (© The Author(s) 2019. Published by Oxford University Press on behalf of the British Society for Rheumatology. All rights reserved. For permissions, please email: journals.permissions@oup.com.)

Published
2019
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41. CD19 + CD24 hi CD38 hi B Cells Are Expanded in Juvenile Dermatomyositis and Exhibit a Pro-Inflammatory Phenotype After Activation Through Toll-Like Receptor 7 and Interferon-α.

Author

Piper CJM, Wilkinson MGL, Deakin CT, Otto GW, Dowle S, Duurland CL, Adams S, Marasco E, Rosser EC, Radziszewska A, Carsetti R, Ioannou Y, Beales PL, Kelberman D, Isenberg DA, Mauri C, Nistala K, and Wedderburn LR

Abstract

Juvenile dermatomyositis (JDM) is a rare form of childhood autoimmune myositis that presents with proximal muscle weakness and skin rash. B cells are strongly implicated in the pathogenesis of the disease, but the underlying mechanisms are unknown. Therefore, the main objective of our study was to investigate mechanisms driving B cell lymphocytosis and define pathological features of B cells in JDM patients. Patients were recruited through the UK JDM Cohort and Biomarker study. Peripheral blood B cell subpopulations were immunophenotyped by flow cytometry. The results identified that immature transitional B cells were significantly expanded in active JDM, actively dividing, and correlated positively with disease activity. Protein and RNAseq analysis revealed high interferon alpha (IFNα) and TLR7-pathway signatures pre-treatment. Stimulation of B cells through TLR7/8 promoted both IL-10 and IL-6 production in controls but failed to induce IL-10 in JDM patient cells. Interrogation of the CD40-CD40L pathway (known to induce B cell IL-10 and IL-6) revealed similar expression of IL-10 and IL-6 in B cells cultured with CD40L from both JDM patients and controls. In conclusion, JDM patients with active disease have a significantly expanded immature transitional B cell population which correlated with the type I IFN signature. Activation through TLR7 and IFNα may drive the expansion of immature transitional B cells in JDM and skew the cells toward a pro-inflammatory phenotype.

Published
2018
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42. Consensus-based recommendations for the management of juvenile dermatomyositis.

Author

Bellutti Enders F, Bader-Meunier B, Baildam E, Constantin T, Dolezalova P, Feldman BM, Lahdenne P, Magnusson B, Nistala K, Ozen S, Pilkington C, Ravelli A, Russo R, Uziel Y, van Brussel M, van der Net J, Vastert S, Wedderburn LR, Wulffraat N, McCann LJ, and van Royen-Kerkhof A

Subjects
Cyclosporine therapeutic use, Dermatomyositis diagnosis, Europe, Evidence-Based Medicine, Humans, Methotrexate therapeutic use, Mycophenolic Acid therapeutic use, Patient Care Team organization & administration, Prednisolone therapeutic use, Rituximab therapeutic use, Societies, Medical, Dermatomyositis therapy, Exercise Therapy, Glucocorticoids therapeutic use, Immunosuppressive Agents therapeutic use, Practice Guidelines as Topic, Sunscreening Agents therapeutic use
Abstract

Background: In 2012, a European initiative called Single Hub and Access point for pediatric Rheumatology in Europe (SHARE) was launched to optimise and disseminate diagnostic and management regimens in Europe for children and young adults with rheumatic diseases. Juvenile dermatomyositis (JDM) is a rare disease within the group of paediatric rheumatic diseases (PRDs) and can lead to significant morbidity. Evidence-based guidelines are sparse and management is mostly based on physicians' experience. Consequently, treatment regimens differ throughout Europe., Objectives: To provide recommendations for diagnosis and treatment of JDM., Methods: Recommendations were developed by an evidence-informed consensus process using the European League Against Rheumatism standard operating procedures. A committee was constituted, consisting of 19 experienced paediatric rheumatologists and 2 experts in paediatric exercise physiology and physical therapy, mainly from Europe. Recommendations derived from a validated systematic literature review were evaluated by an online survey and subsequently discussed at two consensus meetings using nominal group technique. Recommendations were accepted if >80% agreement was reached., Results: In total, 7 overarching principles, 33 recommendations on diagnosis and 19 recommendations on therapy were accepted with >80% agreement among experts. Topics covered include assessment of skin, muscle and major organ involvement and suggested treatment pathways., Conclusions: The SHARE initiative aims to identify best practices for treatment of patients suffering from PRD. Within this remit, recommendations for the diagnosis and treatment of JDM have been formulated by an evidence-informed consensus process to produce a standard of care for patients with JDM throughout Europe., Competing Interests: FBE—Valeria e Ettore Bossi Foundation. EB—speaker bureau for Roche/ Chugai, Ad Board for Abbvie and Pfizer. BMF—consultant for Novartis, Pfizer, BMS. PL—consultant for BMS, Pfizer. SO—consultant for Novartis, speaker bureau of SOBI. PD—consultant for Roche, speaker bureau for Pfizer, Novartis, grant support from SOBI, Novartis, Abbvie, Roche, Pfizer, Medac. AR—grant/research support from Pfizer and The Myositis Association; consultant for Novartis, Roche; speaker bureau of Abbvie, Novartis, Pfizer, Roche. YU—consultant for Novartis, speaker bureau of Abbvie, Neopharm, Novartis, Roche. NW—grant/research support from EAHC, Abbvie, GSK, Roche, consultant for Genzyme, Novartis, Pfizer, Roche, (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/.)

Published
2017
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43. Muscle Biopsy Findings in Combination With Myositis-Specific Autoantibodies Aid Prediction of Outcomes in Juvenile Dermatomyositis.

Author

Deakin CT, Yasin SA, Simou S, Arnold KA, Tansley SL, Betteridge ZE, McHugh NJ, Varsani H, Holton JL, Jacques TS, Pilkington CA, Nistala K, and Wedderburn LR

Subjects
Adrenal Cortex Hormones therapeutic use, Child, Child, Preschool, Cohort Studies, DNA Topoisomerases immunology, DNA-Binding Proteins immunology, Dermatomyositis drug therapy, Dermatomyositis immunology, Female, Humans, Immunosuppressive Agents therapeutic use, Interferon-Induced Helicase, IFIH1 immunology, Longitudinal Studies, Male, Methotrexate therapeutic use, Odds Ratio, Prognosis, Protective Factors, Risk Factors, Severity of Illness Index, Signal Recognition Particle immunology, Threonine-tRNA Ligase immunology, Transcription Factors immunology, United Kingdom, Autoantibodies immunology, Dermatomyositis pathology, Quadriceps Muscle pathology
Abstract

Objective: Juvenile dermatomyositis (DM) is a rare and severe autoimmune condition characterized by rash and proximal muscle weakness. While some patients respond to standard treatment, others do not. This study was carried out to investigate whether histopathologic findings and myositis-specific autoantibodies (MSAs) have prognostic significance in juvenile DM., Methods: Muscle biopsy samples (n = 101) from patients in the UK Juvenile Dermatomyositis Cohort and Biomarker Study were stained, analyzed, and scored for severity of histopathologic features. In addition, autoantibodies were measured in the serum or plasma of patients (n = 90) and longitudinal clinical data were collected (median duration of follow-up 4.9 years). Long-term treatment status (on or off medication over time) was modeled using generalized estimating equations., Results: Muscle biopsy scores differed according to MSA subgroup. When the effects of MSA subgroup were accounted for, increased severity of muscle histopathologic features was predictive of an increased risk of remaining on treatment over time: for the global pathology score (histopathologist's visual analog scale [hVAS] score), 1.48-fold higher odds (95% confidence interval [95% CI] 1.12-1.96; P = 0.0058), and for the total biopsy score (determined with the standardized score tool), 1.10-fold higher odds (95% CI 1.01-1.21; P = 0.038). A protective effect was identified in patients with anti-Mi-2 autoantibodies, in whom the odds of remaining on treatment were 7.06-fold lower (95% CI 1.41-35.36; P = 0.018) despite muscle biopsy scores indicating more severe disease. In patients with anti-nuclear matrix protein 2 autoantibodies, anti-transcription intermediary factor 1γ autoantibodies, or no detectable autoantibody, increased histopathologic severity alone, without adjustment for the effect of MSA subtype, was predictive of the risk of remaining on treatment: for the hVAS global pathology score, 1.61-fold higher odds (95% CI 1.16-2.22; P = 0.004), and for the total biopsy score, 1.13-fold higher odds (95% CI 1.03-1.24; P = 0.013)., Conclusion: Histopathologic severity, in combination with MSA subtype, is predictive of the risk of remaining on treatment in patients with juvenile DM and may be useful for discussing probable treatment length with parents and patients. Understanding these associations may identify patients at greater risk of severe disease., (© 2016 The Authors. Arthritis & Rheumatology published by Wiley Periodicals, Inc. on behalf of the American College of Rheumatology.)

Published
2016
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44. Comparison of the Utility and Validity of Three Scoring Tools to Measure Skin Involvement in Patients With Juvenile Dermatomyositis.

Author

Campanilho-Marques R, Almeida B, Deakin C, Arnold K, Gallot N, de Iorio M, Nistala K, Pilkington CA, and Wedderburn LR

Subjects
Child, Dermatomyositis pathology, Female, Humans, Intention to Treat Analysis, Male, Reproducibility of Results, Skin pathology, Visual Analog Scale, Dermatomyositis diagnosis, Severity of Illness Index, Symptom Assessment methods
Abstract

Objective: To compare the abbreviated Cutaneous Assessment Tool (CAT), Disease Activity Score (DAS), and Myositis Intention to Treat Activity Index (MITAX) and correlate them with the physician's 10-cm skin visual analog scale (VAS) in order to define which tool best assesses skin disease in patients with juvenile dermatomyositis., Methods: A total of 71 patients recruited to the UK Juvenile Dermatomyositis Cohort and Biomarker Study were included and assessed for skin disease using the CAT, DAS, MITAX, and skin VAS. The Childhood Myositis Assessment Scale (CMAS), manual muscle testing of 8 groups (MMT8), muscle enzymes, inflammatory markers, and physician's global VAS were recorded. Relationships were evaluated using Spearman's correlations and predictors with linear regression. Interrater reliability was assessed using intraclass correlation coefficients., Results: All 3 tools showed correlation with the physician's global VAS and skin VAS, with DAS skin showing the strongest correlation with skin VAS. DAS skin and CAT activity were inversely correlated with CMAS and MMT8, but these correlations were moderate. No correlations were found between the skin tools and inflammatory markers or muscle enzymes. DAS skin and CAT were the quickest to complete (mean ± SD 0.68 ± 0.1 minutes and 0.63 ± 0.1 minutes, respectively)., Conclusion: The 3 skin tools were quick and easy to use. The DAS skin correlated best with the skin VAS. The addition of CAT in a bivariate model containing the physician's global VAS was a statistically significant estimator of skin VAS score. We propose that there is scope for a new skin tool to be devised and tested, which takes into account the strengths of the 3 existing tools., (© 2016, The Authors. Arthritis Care & Research published by Wiley Periodicals, Inc. on behalf of the American College of Rheumatology.)

Published
2016
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45. Analysis of Published Criteria for Clinically Inactive Disease in a Large Juvenile Dermatomyositis Cohort Shows That Skin Disease Is Underestimated.

Author

Almeida B, Campanilho-Marques R, Arnold K, Pilkington CA, Wedderburn LR, and Nistala K

Subjects
Adolescent, Child, Cohort Studies, Dermatomyositis blood, Dermatomyositis complications, Female, Humans, Longitudinal Studies, Male, Muscle Strength, Prospective Studies, Skin Diseases etiology, United Kingdom, Calcinosis etiology, Creatine Kinase blood, Dermatomyositis diagnosis, Exanthema etiology, Skin Ulcer etiology
Abstract

Objective: The Pediatric Rheumatology International Trials Organisation (PRINTO) recently published criteria for classification of patients with juvenile dermatomyositis (DM) as having clinically inactive disease. The criteria require that at least 3 of 4 conditions be met, i.e., creatine kinase level ≤150 units/liter, Childhood Myositis Assessment Scale score ≥48, Manual Muscle Testing in 8 muscles score ≥78, and physician's global assessment of overall disease activity (PGA) ≤0.2. The present study was undertaken to test these criteria in a UK cohort of patients with juvenile DM., Methods: We assessed 1,114 patient visits for the 4 items in the PRINTO criteria for clinically inactive disease. Each visit was analyzed to determine whether skin disease was present. The Disease Activity Score (DAS) for juvenile DM was determined in 59 patients., Results: At 307 of the 1,114 visits, clinically inactive disease was achieved based on the 3 muscle criteria (but with a PGA of >0.2); rash was present at 65.8% of these visits and nailfold capillary abnormalities at 35.2%. When PGA ≤0.2 was one of the 3 criteria that were met, the frequency of skin signs was significantly lower (rash in 23.1% and nailfold capillary abnormalities in 8.7%). If PGA was considered an essential criterion for clinically inactive disease (P-CID), patients with active skin disease were less likely to be categorized as having clinically inactive disease (a median DAS skin score of 0 [of a possible maximum of 9] in visits where the PGA was ≤0.2, versus a median DAS skin score of 4 in patients meeting the 3 muscle criteria [with a PGA of >0.2]; P < 0.001). Use of the P-CID led to improvements in the positive predictive value and the positive likelihood ratio (85.4% and 11.0, respectively, compared to 72.9% and 5.1 with the current criteria)., Conclusion: There was a high frequency of skin disease among patients with juvenile DM who did not meet the PGA criterion for inactive disease but met the other 3 criteria. Incorporating PGA as an essential criterion for clinically inactive disease helps prevent the misclassification of patients with active skin disease., (© 2015 The Authors. Arthritis & Rheumatology is published by Wiley Periodicals, Inc. on behalf of the American College of Rheumatology.)

Published
2015
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46. T cell expression of granulocyte-macrophage colony-stimulating factor in juvenile arthritis is contingent upon Th17 plasticity.

Author

Piper C, Pesenacker AM, Bending D, Thirugnanabalan B, Varsani H, Wedderburn LR, and Nistala K

Subjects
Biomarkers metabolism, Cell Differentiation immunology, Cells, Cultured, Child, Female, Granulocyte-Macrophage Colony-Stimulating Factor genetics, Humans, Male, Synovial Fluid immunology, Synovial Fluid metabolism, Th17 Cells cytology, Th17 Cells immunology, Arthritis, Juvenile immunology, Arthritis, Juvenile metabolism, Granulocyte-Macrophage Colony-Stimulating Factor metabolism, Immunity, Innate immunology, Th17 Cells metabolism
Abstract

Objective: Granulocyte-macrophage colony stimulating factor (GM-CSF) is a potent inflammatory mediator that is responsible for recruitment and activation of innate immune cells. Recent data from murine studies have identified Th17 cells as a key source of GM-CSF and suggest that T cell-derived GM-CSF is instrumental in the induction of autoimmune disease. The present study was undertaken to analyze the expression of T cell-derived GM-CSF in the joints of patients with juvenile idiopathic arthritis (JIA) and to investigate the differentiation of Th17 cells and how this relates to GM-CSF+ T helper cells., Methods: Synovial fluid (SF) and peripheral blood (PB) samples from 24 patients with JIA were analyzed, by flow cytometry and reverse transcription-polymerase chain reaction, for expression of GM-CSF and the Th17 marker CD161. A cytokine capture assay was used to purify Th17 cells and test the plasticity of cytokine production in response to interleukin-12 (IL-12) and IL-23., Results: The frequency of GM-CSF-producing T helper cells was significantly enriched in SF mononuclear cells compared to PB mononuclear cells from the patients with JIA (24.1% of CD4+ T cells versus 2.9%) and closely correlated with the erythrocyte sedimentation rate (r(2) = 0.91, P < 0.001). Synovial GM-CSF+ T cells were predominantly CD161+ and coexpressed interferon-γ (IFNγ), but not IL-17. Culture of Th17 cells in the presence of IL-12 led to rapid up-regulation of GM-CSF and IFNγ, recapitulating the phenotype of GM-CSF-expressing cells within the joint., Conclusion: Our results identify a novel outcome of Th17 plasticity in humans that may account for the enrichment of GM-CSF-expressing T cells in the joints of patients with JIA. The association of GM-CSF expression with systemic inflammation highlights the potential role of Th17-related cytokines in the pathology of JIA., (© 2014 The Authors. Arthritis & Rheumatology is published by Wiley Periodicals, Inc. on behalf of the American College of Rheumatology.)

Published
2014
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47. Interleukin-35 takes the 'B' line.

Author

Mauri C and Nistala K

Subjects
Animals, Cytokines immunology, Humans, Immunosuppressive Agents immunology, Interleukins immunology, Mice, Autoimmune Diseases immunology, B-Lymphocytes, Regulatory immunology, Cytokines metabolism, Immunosuppressive Agents metabolism, Interleukins metabolism, Models, Immunological
Published
2014
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48. The quest for personalized B-cell depletion therapy in rheumatic disease.

Author

Nistala K and Mauri C

Subjects
Antirheumatic Agents therapeutic use, Autoantibodies blood, Autoantibodies immunology, B-Lymphocyte Subsets metabolism, Humans, Rheumatic Diseases blood, Rituximab, Treatment Outcome, Antibodies, Monoclonal, Murine-Derived therapeutic use, B-Lymphocyte Subsets immunology, Lymphocyte Depletion methods, Rheumatic Diseases drug therapy, Rheumatic Diseases immunology
Abstract

Although B cell depletion therapy (BCDT) is now a well-accepted therapeutic option in autoimmune rheumatic disease, a significant proportion of patients remain resistant to therapy. .19pt?>A more challenging clinical problem is the high rate of relapse after B cell reconstitution, as well as the difficulty in predicting the exact timing of that relapse. In this article, we consider the immunological mechanisms that may account for the heterogeneity of clinical response to BCDT. Understanding how BCDT alters the balance between different B cell subsets, some pathogenic and some regulatory, may help us correctly target BCDT to the right patients, and thereby improve treatment responses in rheumatic disease.

Published
2014
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49. Update in juvenile myositis.

Author

Nistala K and Wedderburn LR

Subjects
Autoantibodies analysis, Child, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Myositis diagnosis, Myositis therapy, Prognosis, Risk Factors, Sunlight adverse effects, Treatment Outcome, Myositis etiology
Abstract

Purpose of Review: This update on childhood idiopathic inflammatory myopathies (IIMs) reviews recent progress in the field of translational science and clinical research over the past 12-18 months., Recent Findings: Several new studies, including results from the international genome-wide association study, point to abnormalities of the adaptive immune system in childhood IIMs. Circulating T-follicular helper cells promote plasma cell differentiation and have been found in high levels in juvenile dermatomyositis (JDM), which may account the frequency of autoantibodies seen in this disease. One of the latest to be identified in JDM targets the protein NXP-2 and is associated with an increased risk of calcinosis in young patients. The first randomized controlled clinical trial in refractory adult and childhood IIMs was reported this year. B-cell depletion with the anti-CD20 antibody, rituximab, failed to achieve its primary end point, but patients with JDM did show good improvement in disease activity. A new international definition of disease remission in JDM has been agreed, which will aid disease assessment in future therapeutic trials., Summary: The challenges of studying a rare disease such as JDM have been overcome by several collaborative studies and have led to significant progress in understanding the cause, treatment and prognosis of childhood IIMs.

Published
2013
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50. Myeloid related protein induces muscle derived inflammatory mediators in juvenile dermatomyositis.

Author

Nistala K, Varsani H, Wittkowski H, Vogl T, Krol P, Shah V, Mamchaoui K, Brogan PA, Roth J, and Wedderburn LR

Subjects
Adolescent, Antigens, CD metabolism, Antigens, Differentiation, Myelomonocytic metabolism, Biopsy, Calgranulin A blood, Calgranulin B blood, Cell Line, Chemokine CCL2 genetics, Chemokine CCL2 metabolism, Child, Child, Preschool, Cytokines blood, Cytokines metabolism, Dermatomyositis blood, Dermatomyositis pathology, Endoplasmic Reticulum Stress, Female, Gene Expression, Humans, Immunohistochemistry, Interleukin-6 metabolism, Macrophages metabolism, Macrophages pathology, Male, Microscopy, Fluorescence, Muscle Strength, Muscles pathology, Muscles physiopathology, Myoblasts, Skeletal cytology, Myoblasts, Skeletal metabolism, Reverse Transcriptase Polymerase Chain Reaction, Calgranulin A metabolism, Calgranulin B metabolism, Dermatomyositis metabolism, Inflammation Mediators metabolism, Muscles metabolism
Abstract

Introduction: The aetiopathogenesis of juvenile dermatomyositis (JDM) remains poorly understood. In particular the contribution of monocytes or macrophages, which are frequently observed to be an infiltrate within muscle tissue very early in the disease process, is unknown. We hypothesised that these cells secrete the pro-inflammatory myeloid related protein (MRP) 8/14 which may then contribute to muscle pathology in JDM., Methods: In this study of 56 JDM patients, serum MRP8/14 levels were compared with clinical measures of disease activity. Muscle biopsies taken early in disease were assessed by immunohistochemistry to determine the frequency and identity of MRP-expressing cells. The effects of MRP stimulation and endoplasmic reticulum (ER) stress on muscle were tested in vitro. Serum or supernatant levels of cytokines were analyzed by multiplex immunoassay., Results: Serum MRP8/14 correlated with physician's global assessment of disease activity in JDM (R = 0.65, p = 0.0003) and muscle strength/endurance, childhood myositis assessment score (CMAS, R = -0.55, p = 0.004). MRP8/14 was widely expressed by CD68+ macrophages in JDM muscle tissue. When cultured with human myoblasts, MRP8 led to the secretion of MCP-1 and IL-6, which was enhanced by ER stress. Both inflammatory mediators were detected in significantly higher levels in the serum of JDM patients compared to healthy controls., Conclusions: This study is the first to identify serum MRP8/14 as a potential biomarker for disease activity in JDM. We propose that tissue infiltrating macrophages secreting MRP8/14 may contribute to myositis, by driving the local production of cytokines directly from muscle.

Published
2013
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