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2. Positron Emission Tomography to Improve Assessment of Interstitial Lung Disease in Patients With Systemic Sclerosis Eligible for Autologous Stem Cell Transplantation

Author

Broens, B., Laken, C.J. van der, Zwezerijnen, G.J.C., Nossent, E.J., Meijboom, L.J., Spierings, J., Vries-Bouwstra, J.K. de, Laar, J.M. van, Voskuyl, A.E., Rheumatology, AII - Inflammatory diseases, Radiology and nuclear medicine, Pulmonary medicine, CCA - Cancer Treatment and quality of life, AII - Infectious diseases, AMS - Tissue Function & Regeneration, AMS - Musculoskeletal Health, and CCA - Imaging and biomarkers

Subjects
interstitial lung disease, Scleroderma, Systemic, positron emission tomography, systemic sclerosis, Immunology, lung fibrosis, Hematopoietic Stem Cell Transplantation, Transplantation, Autologous, stem cell transplantation, Positron-Emission Tomography, Humans, Immunology and Allergy, scleroderma, Lung Diseases, Interstitial
Abstract

Positron emission tomography (PET) is a promising technique to improve the assessment of systemic sclerosis associated interstitial lung disease (SSc-ILD). This technique could be of particular value in patients with severe diffuse cutaneous SSc (dcSSc) that are possibly eligible for autologous hematopoietic stem cell transplantation (aHSCT). aHSCT is a potentially effective therapy for patients with severe dcSSc and ILD, leading to stabilization or improvement of lung function. However, there is a high need to improve patient selection, which includes (1) the selection of patients with rapidly progressive ILD for early rather than last-resort aHSCT (2) the prediction of treatment response on ILD and (3) the understanding of the mechanism(s) of action of aHSCT in the lungs. As previous studies with 18F-FDG PET in SSc-ILD and other forms of ILD have demonstrated its potential value in predicting disease progression and reactivity to anti-inflammatory treatment, we discuss the potential benefit of using this technique in patients with early severe dcSSc and ILD in the context of aHSCT. In addition, we discuss the potential value of other PET tracers in the assessment of ILD and understanding the mechanisms of action of aHSCT in the lung. Finally, we provide several suggestions for future research.

Published
2022
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3. Identifying relevant determinants of in-hospital time to diagnosis for ANCA-associated vasculitis patients

Author

Dirikgil, E., Tas, S.W., Verburgh, C.A., Soonawala, D., Hak, A.E., Remmelts, H.H.F., IJpelaar, D., Laverman, G.D., Rutgers, A., Laar, J.M. van, Moens, H.J.B., Verhoeven, P.M.J., Rabelink, T.J., Bos, W.J.W., Teng, Y.K.O., Autoimmune Research Collaboration Hub (ARCH) study group, Translational Immunology Groningen (TRIGR), Experimental Immunology, Clinical Immunology and Rheumatology, AII - Inflammatory diseases, and AII - Amsterdam institute for Infection and Immunity

Subjects
DAMAGE, WEGENERS-GRANULOMATOSIS, Rheumatology, patient trajectory, pauci-immune glomerulonephritis, CYCLOPHOSPHAMIDE, MANAGEMENT, RITUXIMAB, REMISSION, health-care usage, ANTIBODY-ASSOCIATED VASCULITIS, ANCA-associated vasculitis, diagnostic delay
Abstract

Objectives Diagnosing patients with ANCA-associated vasculitis (AAV) can be challenging owing to its rarity and complexity. Diagnostic delay can have severe consequences, such as chronic organ damage or even death. Given that few studies have addressed diagnostic pathways to identify opportunities to improve, we performed a clinical audit to evaluate the diagnostic phase. Methods This retrospective, observational study of electronic medical records data in hospitals focused on diagnostic procedures during the first assessment until diagnosis. Results We included 230 AAV patients from nine hospitals. First assessments were mainly performed by a specialist in internal medicine (52%), pulmonology (14%), ENT (13%) or rheumatology (10%). The overall median time to diagnosis was 13 [interquartile range: 2–49] days, and in patients primarily examined by a specialist in internal medicine it was 6 [1–25] days, rheumatology 14 [4–45] days, pulmonology 15 [5–70] days and ENT 57 [16–176] days (P = 0.004). Twenty-two of 31 (71%) patients primarily assessed by a specialist in ENT had non-generalized disease, of whom 14 (64%) had ENT-limited activity. Two hundred and nineteen biopsies were performed in 187 patients (81%). Histopathological support for AAV was observed in 86% of kidney biopsies, 64% of lung biopsies and 34% of ENT biopsies. Conclusion In The Netherlands, AAV is diagnosed and managed predominantly by internal medicine specialists. Diagnostic delay was associated with non-generalized disease and ENT involvement at presentation. Additionally, ENT biopsies had a low diagnostic yield, in contrast to kidney and lung biopsies. Awareness of this should lead to more frequent consideration of AAV and early referral for a multidisciplinary approach when AAV is suspected.

Published
2022

4. Using real-world data to dynamically predict flares during tapering of biological DMARDs in rheumatoid arthritis: development, validation, and potential impact of prediction-aided decisions

Author

Leeuw, M.S. van der, Messelink, M.A., Tekstra, J., Medina, O., Laar, J.M. van, Haitjema, S., Lafeber, F., Veris-van Dieren, J.J., Goes, M.C. van der, Broeder, A.A. den, Welsing, P. M. J., Leeuw, M.S. van der, Messelink, M.A., Tekstra, J., Medina, O., Laar, J.M. van, Haitjema, S., Lafeber, F., Veris-van Dieren, J.J., Goes, M.C. van der, Broeder, A.A. den, and Welsing, P. M. J.

Abstract

Contains fulltext : 249014.pdf (Publisher’s version ) (Open Access), BACKGROUND: Biological disease-modifying antirheumatic drugs (bDMARDs) are effective in the treatment of rheumatoid arthritis. However, as bDMARDs may also lead to adverse events and are expensive, tapering them is of great clinical interest. Tapering according to disease activity-guided dose optimization (DGDO) does not seem to affect long term remission rates, but flares are frequent during this process. Our objective was to develop a model for the prediction of flares during bDMARD tapering using data from routine care and to evaluate its potential clinical impact. METHODS: We used a joint latent class model to repeatedly predict the probability of a flare occurring within the next 3 months. The model was developed using longitudinal data on disease activity (DAS28) and other routine care data from two clinics. Predictive accuracy was assessed in cross-validation and external validation was performed with data from the DRESS (Dose REduction Strategy of Subcutaneous tumor necrosis factor inhibitors) trial. Additionally, we simulated the reduction in number of flares and bDMARD dose when implementing the model as a decision aid during bDMARD tapering in the DRESS trial. RESULTS: Data from 279 bDMARD courses were used for model development. The final model included two latent DAS28-trajectories, bDMARD type and dose, disease duration, and seropositivity. The area under the curve of the final model was 0.76 (0.69-0.83) in cross-validation and 0.68 (0.62-0.73) in external validation. In simulation of prediction-aided decisions, the mean number of flares over 18 months decreased from 1.21 (0.99-1.43) to 0.75 (0.54-0.96). The reduction in he bDMARD dose was mostly maintained, increasing from 54 to 64% of full dose. CONCLUSIONS: We developed a dynamic flare prediction model, exclusively based on data typically available in routine care. Our results show that using this model to aid decisions during bDMARD tapering may significantly reduce the number of flares while maint

Published
2022

5. EULAR points to consider for the management of difficult-to-treat rheumatoid arthritis

Author

Nagy, G., Roodenrijs, N.M.T., Welsing, P. M. J., Kedves, M., Hamar, A., Goes, M.C. van der, Kent, A., Bakkers, M., Pchelnikova, P., Blaas, E., Senolt, L., Szekanecz, Z., Choy, E.H., Dougados, M., Jacobs, J.W.G., Geenen, R., Bijlsma, J.W., Zink, A., Aletaha, D., Schoneveld, L., Riel, P. van, Dumas, S., Prior, Y., Nikiphorou, E., Ferraccioli, G., Schett, G., Hyrich, K.L., Mueller-Ladner, U., Buch, M.H., McInnes, I.B., Heijde, D. van der, Laar, J.M. van, Nagy, G., Roodenrijs, N.M.T., Welsing, P. M. J., Kedves, M., Hamar, A., Goes, M.C. van der, Kent, A., Bakkers, M., Pchelnikova, P., Blaas, E., Senolt, L., Szekanecz, Z., Choy, E.H., Dougados, M., Jacobs, J.W.G., Geenen, R., Bijlsma, J.W., Zink, A., Aletaha, D., Schoneveld, L., Riel, P. van, Dumas, S., Prior, Y., Nikiphorou, E., Ferraccioli, G., Schett, G., Hyrich, K.L., Mueller-Ladner, U., Buch, M.H., McInnes, I.B., Heijde, D. van der, and Laar, J.M. van

Abstract

Item does not contain fulltext, OBJECTIVE: To develop evidence-based European Alliance of Associations for Rheumatology (EULAR) points to consider (PtCs) for the management of difficult-to-treat rheumatoid arthritis (D2T RA). METHODS: An EULAR Task Force was established comprising 34 individuals: 26 rheumatologists, patient partners and rheumatology experienced health professionals. Two systematic literature reviews addressed clinical questions around diagnostic challenges, and pharmacological and non-pharmacological therapeutic strategies in D2T RA. PtCs were formulated based on the identified evidence and expert opinion. Strength of recommendations (SoR, scale A-D: A typically consistent level 1 studies and D level 5 evidence or inconsistent studies) and level of agreement (LoA, scale 0-10: 0 completely disagree and 10 completely agree) of the PtCs were determined by the Task Force members. RESULTS: Two overarching principles and 11 PtCs were defined concerning diagnostic confirmation of RA, evaluation of inflammatory disease activity, pharmacological and non-pharmacological interventions, treatment adherence, functional disability, pain, fatigue, goal setting and self-efficacy and the impact of comorbidities. The SoR varied from level C to level D. The mean LoA with the overarching principles and PtCs was generally high (8.4-9.6). CONCLUSIONS: These PtCs for D2T RA can serve as a clinical roadmap to support healthcare professionals and patients to deliver holistic management and more personalised pharmacological and non-pharmacological therapeutic strategies. High-quality evidence was scarce. A research agenda was created to guide future research.

Published
2022

7. Health-related quality of life in patients with mixed connective tissue diseases

Author

Abouyahya, I., Liem, S.I.E., Amoura, Z., Fonseca, J.E., Chaigne, B., Cutolo, M., Doria, A., Fischer-Betz, R., Guimaraes, V., Huizinga, T.W.J., Laar, J.M. van, Martin, T., Matucci-Cerinic, M., Montecucco, C., Schneider, M., Smith, V., Muller-Ladner, U., and Vries-Bouwstra, J.K. de

Subjects
quality of life, systemic sclerosis, mixed connective tissue disease
Abstract

Objective. Health-Related Quality of Life (HRQoL) in adult patients with mixed connective tissue disease (MCTD) has not been described so far. Therefore, we performed an explorative study to evaluate HRQoL in MCTD patients.Methods. MCTD patients fulfilling the Kahn criteria and participating in the prospective follow-up cohort for MCTD of the Leiden University Medical Center were included; and matched to systemic sclerosis (SSc) patients based on age, sex and disease duration. Data on disease characteristics and HRQoL (SF36 and EQ-5D) were collected annually. HRQoL was compared between MCTD and SSc patients at baseline. Factors associated with HRQoL in MCTD were identified using linear regression and change in HRQoL over 3 years using linear mixed models.Results. Thirty-four MCTD patients (121 visits) and 102 SSc patients (424 visits) were included. At baseline, MCTD patients presented with interstitial lung disease, cardiac involvement, synovitis and myositis more frequently compared to SSc patients, while use of immunosuppressive medication was less frequent. In both groups, mean SF36 scores were lower than in the general Dutch population. The SF36 subscore "general health perception" was impacted most in both groups (MCTD: 38.5 [SD:7.0], SSc: 39.9 [SD:8.9]). During follow-up, SF36 scores improved in MCTD patients, while EQ5DNL remained stable. No specific characteristics were identified that associated with baseline HRQoL or change in HRQol over time.Conclusion. Like in SSc, HRQoL in MCTD is significantly impaired, especially the general health perception of patients. Evaluation in larger prospective cohorts is needed to identify characteristics that impact HRQol most.

Published
2022

8. A randomised, open-label trial to assess the optimal treatment strategy in early diffuse cutaneous systemic sclerosis: the UPSIDE study protocol

Author

Spierings, J., Rhenen, A. van, Welsing, P. M. J., Marijnissen, A.C., Langhe, E. De, Papa, N. Del, Dierickx, D., Gheorghe, K.R., Henes, J., Hesselstrand, R., Kerre, T., Ljungman, P., Loosdrecht, A.A. van de, Marijt, E.W., Mayer, M., Schmalzing, M., Schroers, R., Smith, V., Voll, R.E., Vonk, M.C., Voskuyl, A.E., Vries-Bouwstra, J.K. de, Walker, U.A., Wuttge, D.M., Laar, J.M. van, Spierings, J., Rhenen, A. van, Welsing, P. M. J., Marijnissen, A.C., Langhe, E. De, Papa, N. Del, Dierickx, D., Gheorghe, K.R., Henes, J., Hesselstrand, R., Kerre, T., Ljungman, P., Loosdrecht, A.A. van de, Marijt, E.W., Mayer, M., Schmalzing, M., Schroers, R., Smith, V., Voll, R.E., Vonk, M.C., Voskuyl, A.E., Vries-Bouwstra, J.K. de, Walker, U.A., Wuttge, D.M., and Laar, J.M. van

Abstract

Contains fulltext : 232577.pdf (Publisher’s version ) (Open Access), INTRODUCTION: Systemic sclerosis (SSc) is a chronic, autoimmune connective tissue disease associated with high morbidity and mortality, especially in diffuse cutaneous SSc (dcSSc). Currently, there are several treatments available in early dcSSc that aim to change the disease course, including immunosuppressive agents and autologous haematopoietic stem cell transplantation (HSCT). HSCT has been adopted in international guidelines and is offered in current clinical care. However, optimal timing and patient selection for HSCT are still unclear. In particular, it is unclear whether HSCT should be positioned as upfront therapy or rescue treatment for patients refractory to immunosuppressive therapy. We hypothesise that upfront HSCT is superior and results in lower toxicity and lower long-term medical costs. Therefore, we propose this randomised trial aiming to determine the optimal treatment strategy for early dcSSc by comparing two strategies used in standard care: (1) upfront autologous HSCT versus (2) immunosuppressive therapy (intravenous cyclophosphamide pulse therapy followed by mycophenolate mofetil) with rescue HSCT in case of treatment failure. METHODS AND ANALYSIS: The UPSIDE (UPfront autologous hematopoietic Stem cell transplantation vs Immunosuppressive medication in early DiffusE cutaneous systemic sclerosis) study is a multicentre, randomised, open-label, controlled trial. In total, 120 patients with early dcSSc will be randomised. The primary outcome is event-free survival at 2 years after randomisation. Secondary outcomes include serious adverse events, functional status and health-related quality of life. We will also evaluate changes in nailfold capillaroscopy pattern, pulmonary function, cardiac MR and high-resolution CT of the chest. Follow-up visits will be scheduled 3-monthly for 2 years and annually in the following 3 years. ETHICS AND DISSEMINATION: The study was approved by the Dutch Central Committee on Research Concerning Human Subjects (NL726

Published
2021

9. Microbiome and Inflammation in Antibody Deficiency

Author

Willems, R.J.L., Laar, J.M. van, Leavis, H.L., Ellerbroek, P.M., Berbers, Roos-Marijn, Willems, R.J.L., Laar, J.M. van, Leavis, H.L., Ellerbroek, P.M., and Berbers, Roos-Marijn

Published
2021

10. Difficult-to-treat rheumatoid arthritis

Author

Laar, J.M. van, Lafeber, F.P.J.G., Goes, M.C. van der, Welsing, P.M.J., Roodenrijs, Nadia Maria Theresia, Laar, J.M. van, Lafeber, F.P.J.G., Goes, M.C. van der, Welsing, P.M.J., and Roodenrijs, Nadia Maria Theresia

Published
2021

12. How do patients with systemic sclerosis experience currently provided healthcare and how should we measure its quality?

Author

Spierings, J., Ende, C.H.M. van den, Schriemer, R.M., Moens, H.J.B., Bijl, E.A. van der, Bonte-Mineur, F., Buck, M.P.D. de, Kanter, M.A.E. de, Knaapen-Hans, H.K.A., Laar, J.M. van, Mulder, U.D.J., Potjewijd, J., Pundert, L.A.J. de, Schoonbrood, T.H.M., Schouffoer, A.A., Stel, A.J., Vercoutere, W., Voskuyl, A.E., Vries-Bouwstra, J.K. de, Vonk, M.C., ARCH Study Grp, Rheumatology, MUMC+: MA Nefrologie (9), Interne Geneeskunde, MUMC+: MA Reumatologie (9), RS: FHML non-thematic output, Groningen Kidney Center (GKC), and Translational Immunology Groningen (TRIGR)

Subjects
Male, systemic sclerosis, perspective, Computer-assisted web interviewing, GUIDELINES, NEEDS, patients, healthcare organization, 0302 clinical medicine, quality of care, Surveys and Questionnaires, SCLERODERMA, Health care, Pharmacology (medical), 030212 general & internal medicine, media_common, Netherlands, quality indicators, Clinical Science, Middle Aged, Treatment Outcome, Patient Satisfaction, Female, SET, Adult, medicine.medical_specialty, media_common.quotation_subject, Health Personnel, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, Rheumatology, patient-reported outcome measurement, medicine, Humans, Quality (business), Quality of care, Quality Indicators, Health Care, Quality of Health Care, 030203 arthritis & rheumatology, Physician-Patient Relations, Scleroderma, Systemic, business.industry, Mean age, OUTCOME MEASURES, Physical therapy, Inflammatory diseases Radboud Institute for Health Sciences [Radboudumc 5], Organ involvement, Cq index, business, Time to diagnosis
Abstract

Objectives To gain insight into SSc patients’ perspective on quality of care and to survey their preferred quality indicators. Methods An online questionnaire about healthcare setting, perceived quality of care (CQ index) and quality indicators, was sent to 2093 patients from 13 Dutch hospitals. Results Six hundred and fifty patients (mean age 59 years, 75% women, 32% limited cutaneous SSc, 20% diffuse cutaneous SSc) completed the questionnaire. Mean time to diagnosis was 4.3 years (s.d. 6.9) and was longer in women compared with men (4.8 (s.d. 7.3) vs 2.5 (s.d. 5.0) years). Treatment took place in a SSc expert centre for 58%, regional centre for 29% or in both for 39% of patients. Thirteen percent of patients was not aware of whether their hospital was specialized in SSc. The perceived quality of care was rated with a mean score of 3.2 (s.d. 0.5) (range 1.0–4.0). There were no relevant differences between expert and regional centres. The three prioritized process indicators were: good patient-physician interaction (80%), structural multidisciplinary collaboration (46%) and receiving treatment according to SSc guidelines (44%). Absence of disease progression (66%), organ involvement (33%) and digital ulcers (27%) were the three highest rated outcome indicators. Conclusion The perceived quality of care evaluated in our study was fair to good. No differences between expert and regional centres were observed. Our prioritized process and outcome indicators can be added to indicators suggested by SSc experts in earlier studies and can be used to evaluate the quality of care in SSc.

Published
2020
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13. A Dutch consensus statement on the diagnosis and treatment of ANC A-associated vasculitis

Author

Dirikgil, E., Tas, S.W., Rutgers, A., Verhoeven, P.M.J., Laar, J.M. van, Hagen, E.C., Tekstra, J., Hak, A.E.L., Paassen, P. van, Kok, M.R., Goldschmeding, R., Dam, B. van, Douma, C.E., Remmelts, H.H.F., Sanders, J.F., Jonker, J.T., Rabelink, T.J., Damoiseaux, J.G.M.C., Moens, H.J.B., Bos, W.J.W., Teng, Y.K.O., and Arthrit Res Collaboration Hub Cons

Subjects
viruses, pauci-immune glomerulonephritis, recommendations, ANCA-associated vasculitis
Abstract

Introduction: Despite the availability of several guidelines on the diagnosis and treatment of antineutrophil cytoplasmic antibody-associated vasculitis (AAV), clinical routine practice will only improve when an implementation strategy is in place to support clinical decision making and adequate implementation of guidelines. We describe here an initiative to establish national and multidisciplinary consensus on broad aspects of the diagnosis and treatment of AAV relevant to daily clinical practice in the Netherlands.Methods: A multidisciplinary working group of physicians in the Netherlands with expertise on AAV addressed the broad spectrum of diagnosis, terminology, and immunosuppressive and non-immunosuppressive treatment, including an algorithm for AAV patients. Based on recommendations from (inter)national guidelines, national consensus was established using a Delphi-based method during a conference in conjunction with a nationally distributed online consensus survey. Cut-off for consensus was 70% (dis)agreement.Results: Ninety-eight professionals were involved in the Delphi procedure to assess consensus on 5o statements regarding diagnosis, treatment, and organisation of care for AAV patients. Consensus was achieved for 37/50 statements (74%) in different domains of diagnosis and treatment of AAV including consensus on the treatment algorithm for AAV.Conclusion: We present a national, multidisciplinary consensus on a diagnostic strategy and treatment algorithm for AAV patients as part of the implementation of (inter)national guideline-derived recommendations in the Netherlands. Future studies will focus on evaluating local implementation of treatment protocols for AAV, and assessments of current and future clinical practice variation in the care for AAV patients in the Netherlands.

Published
2020

14. Treatment decision-making in diffuse cutaneous systemic sclerosis: a patient's perspective

Author

Spierings, J., Rhijn-Brouwer, F.C. van, Bresser, C.J.M. de, Mosterman, P.T.M., Pieterse, A.H., Vonk, M.C., Voskuyl, A.E., Vries-Bouwstra, J.K. de, Kars, M.C., Laar, J.M. van, Spierings, J., Rhijn-Brouwer, F.C. van, Bresser, C.J.M. de, Mosterman, P.T.M., Pieterse, A.H., Vonk, M.C., Voskuyl, A.E., Vries-Bouwstra, J.K. de, Kars, M.C., and Laar, J.M. van

Abstract

Contains fulltext : 226034.pdf (Publisher’s version ) (Open Access), OBJECTIVES: To examine the treatment decision-making process of patients with dcSSc in the context of haematopoietic stem cell transplantation (HSCT). METHODS: A qualitative semi-structured interview study was done in patients before or after HSCT, or patients who chose another treatment than HSCT. Thematic analysis was used. Shared decision-making (SDM) was assessed with the 9-item Shared Decision Making Questionnaire (SDM-Q-9). RESULTS: Twenty-five patients [16 male/nine female, median age 47 (range 27-68) years] were interviewed: five pre-HSCT, 16 post-HSCT and four following other treatment. Whereas the SDM-Q-9 showed the decision-making process was perceived as shared [median score 81/100 (range 49-100)], we learned from the interviews that the decision was predominantly made by the rheumatologist, and patients were often steered towards a treatment option. Strong guidance of the rheumatologist was appreciated because of a lack of accessible, reliable and SSc-specific information, due to the approach of the decision-making process of the rheumatologist, the large consequence of the decision and the trust in their doctor. Expectations of outcomes and risks also differed between patients. Furthermore, more than half of patients felt they had no choice but to go for HSCT, due to rapid deterioration of health and the perception of HSCT as 'the holy grail'. CONCLUSION: This is the first study that provides insight into the decision-making process in dcSSc. This process is negatively impacted by a lack of disease-specific education about treatment options. Additionally, we recommend exploring patients' preferences and understanding of the illness to optimally guide decision-making and to provide tailor-made information.

Published
2020

15. Standardisation of nailfold capillaroscopy for the assessment of patients with Raynaud's phenomenon and systemic sclerosis

Author

Smith, V., Herrick, A.L., Ingegnoli, F., Damjanov, N., Angelis, R. De, Denton, C.P., Distler, O., Espejo, K., Foeldvari, I., Frech, T., Garro, B., Gutierrez, M., Gyger, G., Hachulla, E., Hesselstrand, R., Iagnocco, A., Kayser, C., Melsens, K., Muller-Ladner, U., Paolino, S., Pizzorni, C., Radic, M., Riccieri, V., Snow, M., Stevens, W.B.C., Sulli, A., Laar, J.M. van, Vonk, M.C., Vanhaecke, A., Cutolo, M., Smith, V., Herrick, A.L., Ingegnoli, F., Damjanov, N., Angelis, R. De, Denton, C.P., Distler, O., Espejo, K., Foeldvari, I., Frech, T., Garro, B., Gutierrez, M., Gyger, G., Hachulla, E., Hesselstrand, R., Iagnocco, A., Kayser, C., Melsens, K., Muller-Ladner, U., Paolino, S., Pizzorni, C., Radic, M., Riccieri, V., Snow, M., Stevens, W.B.C., Sulli, A., Laar, J.M. van, Vonk, M.C., Vanhaecke, A., and Cutolo, M.

Abstract

Contains fulltext : 219902.pdf (Publisher’s version ) (Open Access), Capillaroscopy is a non-invasive and safe tool which allows the evaluation of the morphology of the microcirculation. Since its recent incorporation in the 2013 American College of Rheumatology (ACR)/European League Against Rheumatism (EULAR) classification criteria for systemic sclerosis together with its assessed role to monitor disease progression, capillaroscopy became a 'mainstream' investigation for rheumatologists. Given its increasing use by a variety of physicians internationally both in daily practice to differentiate primary from secondary Raynaud's phenomenon, as well as in research context to predict disease progression and monitor treatment effects, standardisation in capillaroscopic image acquisition and analysis seems paramount. To step forward to this need, experts in the field of capillaroscopy/microcirculation provide in this very consensus paper their view on image acquisition and analysis, different capillaroscopic techniques, normal and abnormal capillaroscopic characteristics and their meaning, scoring systems and reliability of image acquisition and interpretation.

Published
2020

18. Fast track algorithm: How to differentiate a 'scleroderma pattern' from a 'non-scleroderma pattern'

Author

Smith, V., Vanhaecke, A., Herrick, A.L., Distler, O., Guerra, M.G., Denton, C.P., Deschepper, E., Foeldvari, I., Gutierrez, M., Hachulla, E., Ingegnoli, F., Kubo, S., Muller-Ladner, U., Riccieri, V., Sulli, A., Laar, J.M. van, Vonk, M.C., Walker, U.A., Cutolo, M., Smith, V., Vanhaecke, A., Herrick, A.L., Distler, O., Guerra, M.G., Denton, C.P., Deschepper, E., Foeldvari, I., Gutierrez, M., Hachulla, E., Ingegnoli, F., Kubo, S., Muller-Ladner, U., Riccieri, V., Sulli, A., Laar, J.M. van, Vonk, M.C., Walker, U.A., and Cutolo, M.

Abstract

Contains fulltext : 215793.pdf (publisher's version ) (Open Access), OBJECTIVES: This study was designed to propose a simple "Fast Track algorithm" for capillaroscopists of any level of experience to differentiate "scleroderma patterns" from "non-scleroderma patterns" on capillaroscopy and to assess its inter-rater reliability. METHODS: Based on existing definitions to categorise capillaroscopic images as "scleroderma patterns" and taking into account the real life variability of capillaroscopic images described standardly according to the European League Against Rheumatism (EULAR) Study Group on Microcirculation in Rheumatic Diseases, a fast track decision tree, the "Fast Track algorithm" was created by the principal expert (VS) to facilitate swift categorisation of an image as "non-scleroderma pattern (category 1)" or "scleroderma pattern (category 2)". Mean inter-rater reliability between all raters (experts/attendees) of the 8th EULAR course on capillaroscopy in Rheumatic Diseases (Genoa, 2018) and, as external validation, of the 8th European Scleroderma Trials and Research group (EUSTAR) course on systemic sclerosis (SSc) (Nijmegen, 2019) versus the principal expert, as well as reliability between the rater pairs themselves was assessed by mean Cohen's and Light's kappa coefficients. RESULTS: Mean Cohen's kappa was 1/0.96 (95% CI 0.95-0.98) for the 6 experts/135 attendees of the 8th EULAR capillaroscopy course and 1/0.94 (95% CI 0.92-0.96) for the 3 experts/85 attendees of the 8th EUSTAR SSc course. Light's kappa was 1/0.92 at the 8th EULAR capillaroscopy course, and 1/0.87 at the 8th EUSTAR SSc course. CONCLUSION: For the first time, a clinical expert based fast track decision algorithm has been developed to differentiate a "non-scleroderma" from a "scleroderma pattern" on capillaroscopic images, demonstrating excellent reliability when applied by capillaroscopists with varying levels of expertise versus the principal expert and corroborated with external validation.

Published
2019

19. Autologous stem cell transplantation in the treatment of systemic sclerosis: Report from the EBMT/EULAR Registry

Author

Farge, D., Passweg, J., Laar, J.M. van, Marjanovic, Z., Besenthal, C., Finke, J., Peter, H.H., Breedveld, F.C., Fibbe, W.E., Black, C., Denton, C., Koetter, I., Locatelli, F., Martini, A., Schattenberg, A.V.N., Hoogen, F. van den, Putte, L. van de, Lanza, F., Arnold, R., Bacon, P.A., Bingham, S., Ciceri, F., Didier, B., Diez-Martin, J.L., Emery, P., Feremans, W., Hertenstein, B., Hiepe, F., Luosujarvi, R., Lara, A. Leon, Marmont, A., Martinez, A.M., Cascon, H. Pascual, Bocelli-Tyndall, C., Gluckman, E., Gratwohl, A., and Tyndall, A.

Subjects
Scleroderma (Disease) -- Patient outcomes, Systemic scleroderma -- Patient outcomes, Stem cells -- Transplantation, Stem cells -- Patient outcomes, Stem cells -- Analysis, Health
Published
2004

20. Characteristics of difficult-to-treat rheumatoid arthritis: results of an international survey

Author

Roodenrijs, N.M.T., Hair, M.J.H. de, Goes, M.C. van der, Jacobs, J.W.G., Welsing, P.M.J., Heijde, D. van der, Aletaha, D., Dougados, M., Hyrich, K.L., McInnes, I.B., Mueller-Ladner, U., Senolt, L., Szekanecz, Z., Laar, J.M. van, Nagy, G., and EULAR Recommendations

Subjects
musculoskeletal diseases, 0301 basic medicine, medicine.medical_specialty, Immunology, Comorbidity, Disease, Klinikai orvostudományok, General Biochemistry, Genetics and Molecular Biology, Arthritis, Rheumatoid, Disease activity, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, Prednisone, Surveys and Questionnaires, Humans, Immunology and Allergy, Medicine, Intensive care medicine, 030203 arthritis & rheumatology, Polypharmacy, business.industry, International survey, Orvostudományok, medicine.disease, 030104 developmental biology, Current management, Rheumatoid arthritis, Rheumatologists, business, Rheumatism, medicine.drug
Abstract

ObjectivesPatients with difficult-to-treat rheumatoid arthritis (RA) remain symptomatic despite treatment according to current European League Against Rheumatism (EULAR) management recommendations. These focus on early phases of the disease and pharmacological management. We aimed to identify characteristics of difficult-to-treat RA and issues to be addressed in its workup and management that are not covered by current management recommendations.MethodsAn international survey was conducted among rheumatologists with multiple-choice questions on disease characteristics of difficult-to-treat RA. Using open questions, additional items to be addressed and items missing in current management recommendations were identified.Results410 respondents completed the survey: 50% selected disease activity score assessing 28 joints >3.2 OR presence of signs suggestive of active disease as characteristics of difficult-to-treat RA; 42% selected fatigue; 48% selected failure to ≥2 conventional synthetic disease-modifying antirheumatic drugs (DMARDs) AND ≥2 biological/targeted synthetic DMARDs; 89% selected inability to taper glucocorticoids below 5 mg or 10 mg prednisone equivalent daily. Interfering comorbidities, extra-articular manifestations and polypharmacy were identified as important issues missing in current management recommendations.ConclusionsThere is wide variation in concepts of difficult-to-treat RA. Several important issues regarding these patients are not addressed by current EULAR recommendations.

Published
2018

21. Patterns and predictors of skin score change in early diffuse systemic sclerosis from the European Scleroderma Observational Study

Author

Herrick, A.L., Peytrignet, S., Lunt, M., Pan, X., Hesselstrand, R., Mouthon, L., Silman, A.J., Dinsdale, G., Brown, E., Czirjak, L., Distler, J.H., Distler, O., Fligelstone, K., Gregory, W.J., Ochiel, R., Vonk, M.C., Ancuta, C., Ong, V.H., Farge, D., Hudson, M., Matucci-Cerinic, M., Balbir-Gurman, A., Midtvedt, O., Jobanputra, P., Jordan, A.C., Stevens, W.B.C., Moinzadeh, P., Hall, F.C., Agard, C., Anderson, M.E., Diot, E., Madhok, R., Akil, M., Buch, M.H., Chung, L., Damjanov, N.S., Gunawardena, H., Lanyon, P., Ahmad, Y., Chakravarty, K., Jacobsen, S., MacGregor, A.J., McHugh, N., Muller-Ladner, U., Riemekasten, G., Becker, M., Roddy, J., Carreira, P.E., Fauchais, A.L., Hachulla, E., Hamilton, J., Inanc, M., McLaren, J.S., Laar, J.M. van, Pathare, S., Proudman, S.M., Rudin, A., Sahhar, J., Coppere, B., Serratrice, C., Sheeran, T., Veale, D.J., Grange, C., Trad, G.S., Denton, C.P., Herrick, A.L., Peytrignet, S., Lunt, M., Pan, X., Hesselstrand, R., Mouthon, L., Silman, A.J., Dinsdale, G., Brown, E., Czirjak, L., Distler, J.H., Distler, O., Fligelstone, K., Gregory, W.J., Ochiel, R., Vonk, M.C., Ancuta, C., Ong, V.H., Farge, D., Hudson, M., Matucci-Cerinic, M., Balbir-Gurman, A., Midtvedt, O., Jobanputra, P., Jordan, A.C., Stevens, W.B.C., Moinzadeh, P., Hall, F.C., Agard, C., Anderson, M.E., Diot, E., Madhok, R., Akil, M., Buch, M.H., Chung, L., Damjanov, N.S., Gunawardena, H., Lanyon, P., Ahmad, Y., Chakravarty, K., Jacobsen, S., MacGregor, A.J., McHugh, N., Muller-Ladner, U., Riemekasten, G., Becker, M., Roddy, J., Carreira, P.E., Fauchais, A.L., Hachulla, E., Hamilton, J., Inanc, M., McLaren, J.S., Laar, J.M. van, Pathare, S., Proudman, S.M., Rudin, A., Sahhar, J., Coppere, B., Serratrice, C., Sheeran, T., Veale, D.J., Grange, C., Trad, G.S., and Denton, C.P.

Abstract

Contains fulltext : 191335.pdf (publisher's version ) (Open Access), OBJECTIVES: Our aim was to use the opportunity provided by the European Scleroderma Observational Study to (1) identify and describe those patients with early diffuse cutaneous systemic sclerosis (dcSSc) with progressive skin thickness, and (2) derive prediction models for progression over 12 months, to inform future randomised controlled trials (RCTs). METHODS: The modified Rodnan skin score (mRSS) was recorded every 3 months in 326 patients. 'Progressors' were defined as those experiencing a 5-unit and 25% increase in mRSS score over 12 months (+/-3 months). Logistic models were fitted to predict progression and, using receiver operating characteristic (ROC) curves, were compared on the basis of the area under curve (AUC), accuracy and positive predictive value (PPV). RESULTS: 66 patients (22.5%) progressed, 227 (77.5%) did not (33 could not have their status assessed due to insufficient data). Progressors had shorter disease duration (median 8.1 vs 12.6 months, P=0.001) and lower mRSS (median 19 vs 21 units, P=0.030) than non-progressors. Skin score was highest, and peaked earliest, in the anti-RNA polymerase III (Pol3+) subgroup (n=50). A first predictive model (including mRSS, duration of skin thickening and their interaction) had an accuracy of 60.9%, AUC of 0.666 and PPV of 33.8%. By adding a variable for Pol3 positivity, the model reached an accuracy of 71%, AUC of 0.711 and PPV of 41%. CONCLUSIONS: Two prediction models for progressive skin thickening were derived, for use both in clinical practice and for cohort enrichment in RCTs. These models will inform recruitment into the many clinical trials of dcSSc projected for the coming years. TRIAL REGISTRATION NUMBER: NCT02339441.

Published
2018

22. A randomised placebo-controlled double-blind trial to assess the safety of intramuscular administration of allogeneic mesenchymal stromal cells for digital ulcers in systemic sclerosis: the MANUS Trial protocol

Author

Rhijn-Brouwer, F.C. van, Gremmels, H., Fledderus, J.O., Schuurman, A.H., Bonte-Mineur, F., Vonk, M.C., Voskuyl, A.E., Vries-Bouwstra, J.K. de, Coert, J.H., Radstake, T.R., Laar, J.M. van, Verhaar, M.C., Rhijn-Brouwer, F.C. van, Gremmels, H., Fledderus, J.O., Schuurman, A.H., Bonte-Mineur, F., Vonk, M.C., Voskuyl, A.E., Vries-Bouwstra, J.K. de, Coert, J.H., Radstake, T.R., Laar, J.M. van, and Verhaar, M.C.

Abstract

Contains fulltext : 196898.pdf (publisher's version ) (Open Access), INTRODUCTION: Systemic sclerosis (SSc) is an autoimmune disease characterised by inflammation, fibrosis and vasculopathy. Digital ulcers (DUs) are a frequent manifestation of vasculopathy in patients with SSc. Despite recent advances in pharmacological treatments, DU still have major health and economic implications. As there is currently no proven therapeutic strategy to promote DU healing, new treatments are urgently needed. Mesenchymal stem or stromal cells (MSCs) may provide a novel therapy for DU in SSc, because of their immunomodulatory and vasculoregenerative properties. Allogeneic MSC therapy involves functionally competent MSCs from healthy donors and may be used as 'off-the-shelf' available treatment. This study will evaluate whether allogeneic MSC therapy is a safe and potentially efficacious treatment for DU of SSc. METHODS AND ANALYSIS: The MANUS (Mesenchymal stromal cells for Angiogenesis and Neovascularization in digital Ulcers of Systemic Sclerosis) Trial is a double-blind randomised placebo-controlled trial. 20 patients with SSc with refractory DU will be randomised to receive eight intramuscular injections with either placebo or 50*10(6) MSCs. The primary outcome is the toxicity of the treatment at 12 weeks after administration. Secondary outcomes include (serious) adverse events, number and time to healing of DU, pain, reported hand function, quality of life and SSc disease activity. We will also evaluate changes in nailfold capillaroscopy pattern, as well as biochemical parameters and biomarkers in peripheral blood and skin biopsies. Follow-up visits will be scheduled at 48 hours and 2, 4, 8, 12, 24 and 52 weeks post-treatment. If the results confirm safety, feasibility and potential efficacy, a large multicentre randomised controlled trial with longer follow-up will be initiated focusing on efficacy. ETHICS AND DISSEMINATION: The study has been approved by the Dutch Central Committee on Research Concerning Human Subjects (protocol no: NL51705.00

Published
2018

23. Treatment outcome in early diffuse cutaneous systemic sclerosis: the European Scleroderma Observational Study (ESOS)

Author

Herrick, A.L., Pan, X., Peytrignet, S., Lunt, M., Hesselstrand, R., Mouthon, L., Silman, A., Brown, E., Czirjak, L., Distler, J.H., Distler, O., Fligelstone, K., Gregory, W.J., Ochiel, R., Vonk, M.C., Ancuta, C., Ong, V.H., Farge, D., Hudson, M., Matucci-Cerinic, M., Balbir-Gurman, A., Midtvedt, O., Jordan, A.C., Jobanputra, P., Stevens, W.B.C., Moinzadeh, P., Hall, F.C., Agard, C., Anderson, M.E., Diot, E., Madhok, R., Akil, M., Buch, M.H., Chung, L., Damjanov, N., Gunawardena, H., Lanyon, P., Ahmad, Y., Chakravarty, K., Jacobsen, S., MacGregor, A.J., McHugh, N., Muller-Ladner, U., Riemekasten, G., Becker, M, Roddy, J., Carreira, P.E., Fauchais, A.L., Hachulla, E., Hamilton, J., Inanc, M., McLaren, J.S., Laar, J.M. van, Pathare, S., Proudman, S., Rudin, A., Sahhar, J., Coppere, B., Serratrice, C., Sheeran, T., Veale, D.J., Grange, C., Trad, G.S., Denton, C.P., Herrick, A.L., Pan, X., Peytrignet, S., Lunt, M., Hesselstrand, R., Mouthon, L., Silman, A., Brown, E., Czirjak, L., Distler, J.H., Distler, O., Fligelstone, K., Gregory, W.J., Ochiel, R., Vonk, M.C., Ancuta, C., Ong, V.H., Farge, D., Hudson, M., Matucci-Cerinic, M., Balbir-Gurman, A., Midtvedt, O., Jordan, A.C., Jobanputra, P., Stevens, W.B.C., Moinzadeh, P., Hall, F.C., Agard, C., Anderson, M.E., Diot, E., Madhok, R., Akil, M., Buch, M.H., Chung, L., Damjanov, N., Gunawardena, H., Lanyon, P., Ahmad, Y., Chakravarty, K., Jacobsen, S., MacGregor, A.J., McHugh, N., Muller-Ladner, U., Riemekasten, G., Becker, M, Roddy, J., Carreira, P.E., Fauchais, A.L., Hachulla, E., Hamilton, J., Inanc, M., McLaren, J.S., Laar, J.M. van, Pathare, S., Proudman, S., Rudin, A., Sahhar, J., Coppere, B., Serratrice, C., Sheeran, T., Veale, D.J., Grange, C., Trad, G.S., and Denton, C.P.

Abstract

Contains fulltext : 174691.pdf (publisher's version ) (Open Access), OBJECTIVES: The rarity of early diffuse cutaneous systemic sclerosis (dcSSc) makes randomised controlled trials very difficult. We aimed to use an observational approach to compare effectiveness of currently used treatment approaches. METHODS: This was a prospective, observational cohort study of early dcSSc (within three years of onset of skin thickening). Clinicians selected one of four protocols for each patient: methotrexate, mycophenolate mofetil (MMF), cyclophosphamide or 'no immunosuppressant'. Patients were assessed three-monthly for up to 24 months. The primary outcome was the change in modified Rodnan skin score (mRSS). Confounding by indication at baseline was accounted for using inverse probability of treatment (IPT) weights. As a secondary outcome, an IPT-weighted Cox model was used to test for differences in survival. RESULTS: Of 326 patients recruited from 50 centres, 65 were prescribed methotrexate, 118 MMF, 87 cyclophosphamide and 56 no immunosuppressant. 276 (84.7%) patients completed 12 and 234 (71.7%) 24 months follow-up (or reached last visit date). There were statistically significant reductions in mRSS at 12 months in all groups: -4.0 (-5.2 to -2.7) units for methotrexate, -4.1 (-5.3 to -2.9) for MMF, -3.3 (-4.9 to -1.7) for cyclophosphamide and -2.2 (-4.0 to -0.3) for no immunosuppressant (p value for between-group differences=0.346). There were no statistically significant differences in survival between protocols before (p=0.389) or after weighting (p=0.440), but survival was poorest in the no immunosuppressant group (84.0%) at 24 months. CONCLUSIONS: These findings may support using immunosuppressants for early dcSSc but suggest that overall benefit is modest over 12 months and that better treatments are needed. TRIAL REGISTRATION NUMBER: NCT02339441.

Published
2017

24. Association of MicroRNA-618 Expression With Altered Frequency and Activation of Plasmacytoid Dendritic Cells in Patients With Systemic Sclerosis

Author

Rossato, M., Affandi, A.J., Thordardottir, S., Wichers, C.G.K., Cossu, M., Broen, J.C., Moret, F.M., Bossini-Castillo, L., Chouri, E., Bon, L. van, Wolters, F., Marut, W., Kroef, M. van der, Silva-Cardoso, S., Bekker, C.P.J., Dolstra, H., Laar, J.M. van, Martin, J., Roon, J.A.G. van, Reedquist, K.A., Beretta, L., Radstake, T.R., Rossato, M., Affandi, A.J., Thordardottir, S., Wichers, C.G.K., Cossu, M., Broen, J.C., Moret, F.M., Bossini-Castillo, L., Chouri, E., Bon, L. van, Wolters, F., Marut, W., Kroef, M. van der, Silva-Cardoso, S., Bekker, C.P.J., Dolstra, H., Laar, J.M. van, Martin, J., Roon, J.A.G. van, Reedquist, K.A., Beretta, L., and Radstake, T.R.

Abstract

Contains fulltext : 177298.pdf (publisher's version ) (Closed access), OBJECTIVE: Plasmacytoid dendritic cells (PDCs) are a critical source of type I interferons (IFNs) that can contribute to the onset and maintenance of autoimmunity. Molecular mechanisms leading to PDC dysregulation and a persistent type I IFN signature are largely unexplored, especially in patients with systemic sclerosis (SSc), a disease in which PDCs infiltrate fibrotic skin lesions and produce higher levels of IFNalpha than those in healthy controls. This study was undertaken to investigate potential microRNA (miRNA)-mediated epigenetic mechanisms underlying PDC dysregulation and type I IFN production in SSc. METHODS: We performed miRNA expression profiling and validation in highly purified PDCs obtained from the peripheral blood of 3 independent cohorts of healthy controls and SSc patients. Possible functions of miRNA-618 (miR-618) on PDC biology were identified by overexpression in healthy PDCs. RESULTS: Expression of miR-618 was up-regulated in PDCs from SSc patients, including those with early disease who did not present with skin fibrosis. IFN regulatory factor 8, a crucial transcription factor for PDC development and activation, was identified as a target of miR-618. Overexpression of miR-618 reduced the development of PDCs from CD34+ cells in vitro and enhanced their ability to secrete IFNalpha, mimicking the PDC phenotype observed in SSc patients. CONCLUSION: Up-regulation of miR-618 suppresses the development of PDCs and increases their ability to secrete IFNalpha, potentially contributing to the type I IFN signature observed in SSc patients. Considering the importance of PDCs in the pathogenesis of SSc and other diseases characterized by a type I IFN signature, miR-618 potentially represents an important epigenetic target to regulate immune system homeostasis in these conditions.

Published
2017

26. Exploring the inflammatory metabolomic profile to predict response to TNF-α inhibitors in rheumatoid arthritis

Author

Cuppen, B.V.J., Fu, J., Wietmarschen, H.A. van, Harms, A.C., Koval, S., Marijnissen, A.C.A., Peeters, J.J.W., Bijlsma, J.W.J., Tekstra, J., Laar, J.M. van, Hankemeier, T., Lafeber, F.P.J.G., and Greef, J. van der

Subjects
MSB - Microbiology and Systems Biology, Life, Biomedical Innovation, ELSS - Earth, Life and Social Sciences, Biology, Healthy Living
Abstract

In clinical practice, approximately one-Third of patients with rheumatoid arthritis(RA) respond insufficiently to TNF-α inhibitors (TNFis). The aim of the study was to explore the use of a metabolomics to identify predictors for the outcome of TNFi therapy, and study the metabolomic fingerprint in active RA irrespective of patients' response. In the metabolomic profiling, lipids, oxylipins, and amines were measured in serum samples of RA patients from the observational BiOCURA cohort, before start of biological treatment. Multivariable logistic regression models were established to identify predictors for good-and non-response in patients receiving TNFi (n = 124). The added value of metabolites over prediction using clinical parameters only was determined by comparing the area under receiver operating characteristic curve (AUC-ROC), sensitivity, specificity, positive-and negative predictive value and by the net reclassification index (NRI). The models were further validated by 10-fold cross validation and tested on the complete TNFi treatment cohort including moderate responders. Additionally, metaboliteswere identified that cross-sectionally associated with the RA disease activity score based on a 28-joint count (DAS28), erythrocyte sedimentation rate (ESR) or C-reactive protein (CRP). Out of 139 metabolites, the best-performing predictors were sn1-LPC(18:3-ω3/ω6), sn1-LPC(15:0), ethanolamine, and lysine. The model that combined the selected metabolites with clinical parameters showed a significant larger AUC-ROC than that of the model containing only clinical parameters (p = 0.01). The combined model was able to discriminate good-and non-responders with good accuracy and to reclassify non-responders with an improvement of 30% (total NRI = 0.23) and showed a prediction error of 0.27. For the complete TNFi cohort, the NRI was 0.22. In addition, 88 metaboliteswere associated with DAS28, ESR or CRP (p

Published
2016

27. Implication of IL-2/IL-21 region in systemic sclerosis genetic susceptibility

Author

Diaz-Gallo, L.M., Simeon, C.P., Broen, J.C.A., Ortego-Centeno, N., Beretta, L., Vonk, M.C., Carreira, P.E., Vargas, S., Roman-Ivorra, J.A., Gonzalez-Gay, M.A., Tolosa, C., Lopez-Longo, F.J., Espinosa, G., Vicente, E.F., Hesselstrand, R., Riemekasten, G., Witte, T. de, Distler, J.H., Voskuyl, A.E., Schuerwegh, A.J., Shiels, P.G., Nordin, A., Padyukov, L., Hoffmann-Vold, A.M., Scorza, R., Lunardi, C., Airo, P., Laar, J.M. van, Hunzelmann, N., Gathof, B.S., Kreuter, A., Herrick, A., Worthington, J., Denton, C.P., Zhou, X., Arnett, F.C., Fonseca, C., Koeleman, B.P., Assasi, S., Radstake, T.R.D.J., Mayes, M.D., Martin, J., Universitat de Barcelona, Rheumatology, and CCA - Immuno-pathogenesis

Subjects
Male, Genotype, systemic sclerosis, Autoimmune diseases, Immunology, Locus (genetics), Single-nucleotide polymorphism, Genome-wide association study, Biology, Polymorphism, Single Nucleotide, Article, White People, General Biochemistry, Genetics and Molecular Biology, GWAS, IL-2/IL-21 region, Gene Frequency, Rheumatology, Scleroderma, Limited, Medizinische Fakultät, Genetic variation, Genetics, Genetic predisposition, Humans, Immunology and Allergy, Genetic Predisposition to Disease, ddc:610, Allele, Allele frequency, Scleroderma, Systemic, Malalties autoimmunitàries, Interleukins, Logistic Models, Scleroderma (Disease), Case-Control Studies, Scleroderma, Diffuse, Interleukin-2, Evaluation of complex medical interventions Auto-immunity, transplantation and immunotherapy [NCEBP 2], Female, Gene polymorphism, Esclerodèrmia, Genètica
Abstract

ObjectiveThe interleukin 2 (IL-2) and interleukin 21 (IL-21) locus at chromosome 4q27 has been associated with several autoimmune diseases, and both genes are related to immune system functions. The aim of this study was to evaluate the role of the IL-2/IL-21 locus in systemic sclerosis (SSc).Patients and methodsThe case control study included 4493 SSc Caucasian patients and 5856 healthy controls from eight Caucasian populations (Spain, Germany, The Netherlands, USA, Italy, Sweden, UK and Norway). Four single nucleotide polymorphisms (rs2069762, rs6822844, rs6835457 and rs907715) were genotyped using TaqMan allelic discrimination assays.ResultsWe observed evidence of association of the rs6822844 and rs907715 variants with global SSc (pc=6.6E-4 and pc=7.2E-3, respectively). Similar statistically significant associations were observed for the limited cutaneous form of the disease. The conditional regression analysis suggested that the most likely genetic variation responsible for the association was the rs6822844 polymorphism. Consistently, the rs2069762A-rs6822844T-rs6835457G-rs907715T allelic combination showed evidence of association with SSc and limited cutaneous SSc subtype (pc=1.7E-03 and pc=8E-4, respectively).ConclusionsThese results suggested that the IL-2/IL-21 locus influences the genetic susceptibility to SSc. Moreover, this study provided further support for the IL-2/IL-21 locus as a common genetic factor in autoimmune diseases.

Published
2012
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28. Autologous Hematopoietic Stem Cell Transplantation vs Intravenous Pulse Cyclophosphamide in Diffuse Cutaneous Systemic Sclerosis A Randomized Clinical Trial

Author

Laar, J.M. van, Farge, D., Sont, J.K., Naraghi, K., Marjanovic, Z., Larghero, J., Schuerwegh, A.J., Marijt, E.W.A., Vonk, M.C., Schattenberg, A.V., Matucci-Cerinic, M., Voskuyl, A.E., Loosdrecht, A.A. van de, Daikeler, T., Kotter, I., Schmalzing, M., Martin, T., Lioure, B., Weiner, S.M., Kreuter, A., Deligny, C., Durand, J.M., Emery, P., Machold, K.R., Sarrot-Reynauld, F., Warnatz, K., Adoue, D.F.P., Constans, J., Tony, H.P., Papa, N. del, Fassas, A., Himsel, A., Launay, D., Monaco, A. lo, Philippe, P., Quere, I., Rich, E., Westhovens, R., Griffiths, B., Saccardi, R., Hoogen, F.H. van den, Fibbe, W.E., Socie, G., Gratwohl, A., Tyndall, A., EBMT EULAR Scleroderma Study Grp, Rheumatology, Hematology, and CCA - Innovative therapy

Subjects
medicine.medical_specialty, Cyclophosphamide, business.industry, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], medicine.medical_treatment, Hazard ratio, General Medicine, Hematopoietic stem cell transplantation, 3. Good health, Surgery, law.invention, Clinical trial, Transplantation, Autologous stem-cell transplantation, Randomized controlled trial, law, Internal medicine, Inflammatory diseases Radboud Institute for Health Sciences [Radboudumc 5], medicine, Clinical endpoint, business, medicine.drug
Abstract

Contains fulltext : 136804.pdf (Publisher’s version ) (Open Access) IMPORTANCE: High-dose immunosuppressive therapy and autologous hematopoietic stem cell transplantation (HSCT) have shown efficacy in systemic sclerosis in phase 1 and small phase 2 trials. OBJECTIVE: To compare efficacy and safety of HSCT vs 12 successive monthly intravenous pulses of cyclophosphamide. DESIGN, SETTING, AND PARTICIPANTS: The Autologous Stem Cell Transplantation International Scleroderma (ASTIS) trial, a phase 3, multicenter, randomized (1:1), open-label, parallel-group, clinical trial conducted in 10 countries at 29 centers with access to a European Group for Blood and Marrow Transplantation-registered transplant facility. From March 2001 to October 2009, 156 patients with early diffuse cutaneous systemic sclerosis were recruited and followed up until October 31, 2013. INTERVENTIONS: HSCT vs intravenous pulse cyclophosphamide. MAIN OUTCOMES AND MEASURES: The primary end point was event-free survival, defined as time from randomization until the occurrence of death or persistent major organ failure. RESULTS: A total of 156 patients were randomly assigned to receive HSCT (n = 79) or cyclophosphamide (n = 77). During a median follow-up of 5.8 years, 53 events occurred: 22 in the HSCT group (19 deaths and 3 irreversible organ failures) and 31 in the control group (23 deaths and 8 irreversible organ failures). During the first year, there were more events in the HSCT group (13 events [16.5%], including 8 treatment-related deaths) than in the control group (8 events [10.4%], with no treatment-related deaths). At 2 years, 14 events (17.7%) had occurred cumulatively in the HSCT group vs 14 events (18.2%) in the control group; at 4 years, 15 events (19%) had occurred cumulatively in the HSCT group vs 20 events (26%) in the control group. Time-varying hazard ratios (modeled with treatment x time interaction) for event-free survival were 0.35 (95% CI, 0.16-0.74) at 2 years and 0.34 (95% CI, 0.16-0.74) at 4 years. CONCLUSIONS AND RELEVANCE: Among patients with early diffuse cutaneous systemic sclerosis, HSCT was associated with increased treatment-related mortality in the first year after treatment. However, HCST conferred a significant long-term event-free survival benefit. TRIAL REGISTRATION: isrctn.org Identifier: ISRCTN54371254.

Published
2014
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30. Biochemical markers of joint tissue damage increase shortly after a joint bleed; an explorative human and canine in vivo study

Author

Vulpen, L.F. van, Meegeren, M.E. van, Roosendaal, G., Jansen, N.W., Laar, J.M. van, Schutgens, R.E., Mastbergen, S.C., Lafeber, F.P., Vulpen, L.F. van, Meegeren, M.E. van, Roosendaal, G., Jansen, N.W., Laar, J.M. van, Schutgens, R.E., Mastbergen, S.C., and Lafeber, F.P.

Abstract

Item does not contain fulltext, OBJECTIVE: Evaluation whether biomarkers of joint damage are sensitive to change shortly after a joint bleed in hemophilia patients and in a canine model of blood-induced joint damage. METHODS: Blood and urine samples were collected from 10 hemophilia patients after they reported a joint bleed: within 2 days, after 3-5 days, and 12-14 days. Additionally, 90 days after the bleed a blood and urine sample was taken and considered to represent baseline condition. Commercial serum and urine biomarker assays were performed: urinary C-terminal telopeptide of type II collagen (uCTX-II), serum cartilage oligomeric matrix protein (sCOMP), serum cartilage cleavage product C1,2C, and serum chondroitin sulfate 846 (sCS846). The same panel of biomarkers was explored in dogs (n = 7) after induction of a first joint bleed by intra-articular blood injections. Biosamples were collected at baseline, day 2, 1 and 2 weeks later. RESULTS: In hemophilia patients, levels of uCTX-II and sCS846 increased 5 days after joint bleeding when compared with baseline (+52%; P = 0.021 and +14%; P = 0.011, respectively). In dogs, uCTX-II increased statistically significant from day 2 to day 7 (from 75% to 155% of baseline; P = 0.018), and sCOMP from baseline to day 2 (+46%; P = 0.028). CONCLUSIONS: This study demonstrates that biochemical markers of joint tissue damage increase shortly after a single joint bleed, both in humans with established hemophilic arthropathy (HA) and in an animal model of joint damage upon a first joint bleed. Biomarkers might be useful in monitoring the impact of a joint bleed and in evaluation of treatment of such bleeds.

Published
2015

31. A multicenter study confirms CD226 gene association with systemic sclerosis-related pulmonary fibrosis

Author

Bossini-Castillo, L., Simeon, C.P., Beretta, L., Broen, J.C., Vonk, M.C., Rios-Fernandez, R., Espinosa, G., Carreira, P., Camps, M.T., Castillo, M.J., Gonzalez-Gay, M.A., Beltran, E., Freire, M.D., Narvaez, J., Tolosa, C., Witte, T., Kreuter, A., Schuerwegh, A.J., Hoffmann-Vold, A.M., Hesselstrand, R., Lunardi, C., Laar, J.M. van, Chee, M.M., Herrick, A., Koeleman, B.P.C., Denton, C.P., Fonseca, C., Radstake, T.R.D.J., Martin, J., Spanish Scleroderma Grp, The Spanish Scleroderma Group, [Bossini-Castillo,L, Martín,J] Instituto de Parasitología y Biomedicina López-Neyra, IPBLN-CSIC, Granada, Spain. [Simeon,CP] Servicio de Medicina Interna, Hospital Valle de Hebron, Barcelona, Spain. [Beretta,L] IRCCS Fondazione Policlinico-Mangiagalli-Regina Elena and University of Milan, Allergy, Clinical Immunology and Rheumatology, Milan, Italy. [Broen,JC, Vonk,MC] Department of Rheumatology, Radboud University Nijmegen Medical CentreNijmegen, The Netherlands. [Ríos-Fernández,R] Servicio de Medicina Interna, Hospital Clínico Universitario, Granada, Spain. [Espinosa,G] Servicio de Enfermedades Autoinmunes, Hospital Clinic, Barcelona, Spain. [Carreira,P] Servicio de Reumatología, Hospital 12 de Octubre, Madrid, Spain. [Camps,MT] Servicio de Medicina Interna, Hospital Carlos Haya, Málaga, Spain. [Castillo,MJ] Servicio de Medicina Interna, Hospital Virgen del Rocío, Sevilla, Spain. [González-Gay,MA] Servicio de Reumatología, Hospital Universitario Marqués de Valdecilla, IFIMAV, Santander, Spain. [Beltran,E] Servicio de Reumatología, Hospital del Doctor Peset Aleixandre, Valencia, Spain. [Freire,M del C] Unidad Trombosis y Vasculitis, Servicio de Medicina Interna, Hospital Xeral-Complexo Hospitalario Universitario de Vigo, Vigo, Spain. [Narváez,J] Servicio de Reumatología, Hospital Universitario de Bellvitge, Barcelona, Spain. [Tolosa,C] Servicio de Medicina Interna, Hospital Parc Taulí, Sabadell, Spain. [Witte,T] Hannover Medical School, Hannover, Germany. [Kreuter,A] Ruhr University of Bochum, Bochum, Germany. [Schuerwegh,AJ] Department of Rheumatology, Leiden University Medical Center, Leiden, The Netherlands. [Hoffmann-Vold,A-M] Department of Rheumatology, Rikshospitalet, Oslo University Hospital, Rikshospitalet-Radiumhospitalet Medical Center, Oslo, Norway. [Hesselstrand,R] Department of Rheumatology, Lund University, Lund, Sweden. [Lunardi,C] Department of Medicine, Università degli Studi di Verona Verona, Italy. [Van Laar,JM] Institute of Cellular Medicine, Newcastle University, NewcastleUK. [Chee,MM] Centre for Rheumatic Diseases, Glasgow Royal Infirmary, Glasgow, UK. [Herrick,A] Arthritis Research UK Epidemiology Unit, The University of Manchester, Manchester Academic Health Science Centre, Manchester, UK. [Koeleman,BPC] Section Complex Genetics, Department of Medical Genetics, University Medical Center Utrecht, Utrecht, The Netherlands. [Denton,CP, Fonseca,C] Centre for Rheumatology, Royal Free and University College Medical School, University College London, London, UK. [Radstake,TRDJ] Department of Rheumatology and Clinical Immunology, University Medical Center Utrecht, Utrecht, The Netherlands., This work was supported by the following grants: GENFER from the Spanish Society of Rheumatology, SAF2009-11110 from the Spanish Ministry of Science, CTS-4977 from Junta de Andalucía, Spain, in part by Redes Temáticas de Investigación Cooperativa Sanitaria Program, RD08/0075 (RIER) from Instituto de Salud Carlos III (ISCIII), Spain and by Fondo Europeo de Desarrollo Regional (FEDER). The VIDI laureate from the Dutch Association of Research (NWO) and Dutch Arthritis Foundation (National Reumafonds). The Orphan Disease Program grant from the European League Against Rheumatism (EULAR). The Dutch Diabetes Research Foundation (grant 2008.40.001) and the Dutch Arthritis Foundation (Reumafonds, grant NR 09-1-408). DFG WI 1031/6.1. This study was also funded by PI-0590-2010, Consejería de Salud, Junta de Andalucía, Spain., and Universitat de Barcelona

Subjects
Antigens, Differentiation, T-Lymphocyte, Male, systemic sclerosis, CD226 gene, Autoimmune diseases, Pulmonary Fibrosis, Genome-wide association study, Chemicals and Drugs::Biological Factors::Biological Markers::Antigens, Differentiation::Antigens, Differentiation, T-Lymphocyte [Medical Subject Headings], GWAS, Genoma humà, Analytical, Diagnostic and Therapeutic Techniques and Equipment::Investigative Techniques::Genetic Techniques::Genetic Association Studies [Medical Subject Headings], Diseases::Skin and Connective Tissue Diseases::Connective Tissue Diseases::Scleroderma, Systemic [Medical Subject Headings], Organisms::Eukaryota::Animals::Chordata::Vertebrates::Mammals::Primates::Haplorhini::Catarrhini::Hominidae::Humans [Medical Subject Headings], Cohort Studies, Pulmonary fibrosis, Immunology and Allergy, Antígenos de diferenciación de linfocitos T, Malalties autoimmunitàries, Fibrosi pulmonar, Infection and autoimmunity Auto-immunity, transplantation and immunotherapy [NCMLS 1], Evaluation of complex medical interventions Auto-immunity, transplantation and immunotherapy [NCEBP 2], Female, Phenomena and Processes::Genetic Phenomena::Genotype [Medical Subject Headings], Phenomena and Processes::Genetic Phenomena::Genetic Variation [Medical Subject Headings], Research Article, Genotype, Estudios de cohortes, Fibrosis pulmonar, Esclerodermia sistémica, Immunology, Check Tags::Male [Medical Subject Headings], Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Rheumatology, Genetic variation, medicine, Genetic predisposition, Humans, SNP, Diseases::Respiratory Tract Diseases::Lung Diseases::Pulmonary Fibrosis [Medical Subject Headings], Genetic Association Studies, Phenomena and Processes::Genetic Phenomena::Genetic Variation::Polymorphism, Genetic::Polymorphism, Single Nucleotide [Medical Subject Headings], Scleroderma, Systemic, Human genome, Estudios de asociación genética, Haplotype, Autoantibody, Genetic Variation, medicine.disease, Scleroderma (Disease), Check Tags::Female [Medical Subject Headings], Analytical, Diagnostic and Therapeutic Techniques and Equipment::Investigative Techniques::Epidemiologic Methods::Epidemiologic Study Characteristics as Topic::Epidemiologic Studies::Cohort Studies [Medical Subject Headings], Esclerodèrmia, Genotipo
Abstract

Introduction CD226 genetic variants have been associated with a number of autoimmune diseases and recently with systemic sclerosis (SSc). The aim of this study was to test the influence of CD226 loci in SSc susceptibility, clinical phenotypes and autoantibody status in a large multicenter European population. Methods A total of seven European populations of Caucasian ancestry were included, comprising 2,131 patients with SSc and 3,966 healthy controls. Three CD226 single nucleotide polymorphisms (SNPs), rs763361, rs3479968 and rs727088, were genotyped using Taqman 5'allelic discrimination assays. Results Pooled analyses showed no evidence of association of the three SNPs, neither with the global disease nor with the analyzed subphenotypes. However, haplotype block analysis revealed a significant association for the TCG haplotype (SNP order: rs763361, rs34794968, rs727088) with lung fibrosis positive patients (P Bonf = 3.18E-02 OR 1.27 (1.05 to 1.54)). Conclusion Our data suggest that the tested genetic variants do not individually influence SSc susceptibility but a CD226 three-variant haplotype is related with genetic predisposition to SSc-related pulmonary fibrosis., This work was supported by the following grants: JM was funded by GEN-FER from the Spanish Society of Rheumatology, SAF2009-11110 from the Spanish Ministry of Science, CTS-4977 from Junta de Andalucía, Spain, in part by Redes Temáticas de Investigación Cooperativa Sanitaria Program, RD08/0075 (RIER) from Instituto de Salud Carlos III (ISCIII), Spain and by Fondo Europeo de Desarrollo Regional (FEDER).

Published
2012

32. Improvement in Signs and Symptoms of Active Ankylosing Spondylitis Following Treatment with Anti-Interleukin (IL)-17A Monoclonal Antibody Secukinumab Are Paralleled by Reductions in Acute Phase Markers and Inflammatory Markers S100A8 and A9 (Calgranulin A and B)

Author

Baeten, D.L., Bek, S., Wei, J.W., Brachat, A., Sieper, J., Emery, P., Braun, J., Heijde, D. van der, McInnes, I.B., Laar, J.M. van, Landewe, R., Wordsworth, P., Wollenhaupt, J., Kellner, H., Paramarta, J.E., Bertolino, A., Wright, A., and Wolfgang, H.

Published
2012

33. The autoimmune disease-associated IL2RA locus is involved in the clinical manifestations of systemic sclerosis

Author

Martin, J.E., Carmona, F.D., Broen, J.C.A., Simeon, C.P., Vonk, M.C., Carreira, P., Rios-Fernandez, R., Espinosa, G., Vicente-Rabaneda, E., Tolosa, C., Garcia-Hernandez, F.J., Castellvi, I., Fonollosa, V., Gonzalez-Gay, M.A., Saez-Comet, L., Portales, R.G., Pena, P.G. de la, Fernandez-Castro, M., Diaz, B., Martinez-Estupinan, L., Coenen, M., Voskuyl, A.E., Schuerwegh, A.J., Vanthuyne, M., Houssiau, F., Smith, V., Keyser, F. de, Langhe, E. de, Riemekasten, G., Witte, T., Hunzelmann, N., Kreuter, A., Palm, O., Chee, M.M., Laar, J.M. van, Denton, C., Herrick, A., Worthington, J., Koeleman, B.P.C., Radstake, T.R.D.J., Fonseca, C., Martin, J., Spanish Scleroderma Grp, Rheumatology, and CCA - Innovative therapy

Subjects
Adult, Interleukin 2, systemic sclerosis, Immunology, PATHOGENESIS, BETA, Genome-wide association study, Locus (genetics), Biology, Polymorphism, Single Nucleotide, anti-centromere auto-antibody, CLASSIFICATION, Autoimmune Diseases, Immune tolerance, Pathogenesis, INTERLEUKIN-2-RECEPTOR, SCLERODERMA, rs12722495, Genetics, medicine, Medicine and Health Sciences, Humans, REGULATORY T-CELLS, Allele, GENOME-WIDE ASSOCIATION, skin and connective tissue diseases, Genomic disorders and inherited multi-system disorders Molecular epidemiology [IGMD 3], Genetics (clinical), Autoimmune disease, Scleroderma, Systemic, IL2RA, rs2104286, Interleukin-2 Receptor alpha Subunit, Odds ratio, Middle Aged, medicine.disease, Infection and autoimmunity Auto-immunity, transplantation and immunotherapy [NCMLS 1], Genetic Loci, rs11594656, Evaluation of complex medical interventions Auto-immunity, transplantation and immunotherapy [NCEBP 2], medicine.drug
Abstract

Contains fulltext : 109760.pdf (Publisher’s version ) (Closed access) Regulatory T cells (T(regs)) are crucial in the maintenance of the immune tolerance and seem to have an important role in systemic sclerosis (SSc). The interleukin 2 receptor alpha (IL2RA) is an important T(reg) marker, and polymorphisms of IL2RA gene are associated with a number of autoimmune diseases. Therefore, we aimed to investigate for the first time the association of the IL2RA locus in SSc. For this purpose, a total of 3023 SSc patients and 2735 matched healthy controls, from six European Caucasian cohorts, were genotyped for the IL2RA gene variants rs11594656, rs2104286 and rs12722495 using the TaqMan allelic discrimination technology. The overall meta-analysis reached statistical significance when the three polymorphisms were tested for association with SSc, the limited subtype (lcSSc) and anti-centromere auto-antibodies (ACAs). However, no significant P-values were obtained when the ACA-positive patients were removed from the SSc and lcSSc groups, suggesting that these associations rely on ACA positivity. The strongest association signal with ACA production was detected for rs2104286 (P(FDR)=2.07 x 10(-4), odds ratio=1.30 (1.14-1.47)). The associations of rs11594656 and rs12722495 were lost after conditioning to rs2104286, and allelic combination tests did not evidence a combined effect, indicating that rs2104286 best described the association between IL2RA and ACA presence in SSc. 01 februari 2012

Published
2012
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34. A GWAS follow-up study reveals the association of the IL12RB2 gene with systemic sclerosis in Caucasian populations

Author

Bossini-Castillo, L., Martin, J.E., Broen, J., Gorlova, O., Simeon, C.P., Beretta, L., Vonk, M.C., Callejas, J.L., Castellvi, I., Carreira, P., Garcia-Hernandez, F.J., Castro, M.F., Coenen, M.J.H., Riemekasten, G., Witte, T., Hunzelmann, N., Kreuter, A., Distler, J.H.W., Koeleman, B.P., Voskuyl, A.E., Schuerwegh, A.J., Palm, O., Hesselstrand, R., Nordin, A., Airo, P., Lunardi, C., Scorza, R., Shiels, P., Laar, J.M. van, Herrick, A., Worthington, J., Denton, C., Tan, F.K., Arnett, F.C., Agarwal, S.K., Assassi, S., Fonseca, C., Mayes, M.D., Radstake, T.R.D.J., Martin, J., Spanish Scleroderma Grp, Rheumatology, and CCA - Immuno-pathogenesis

Subjects
medicine.medical_specialty, SNP, Single-nucleotide polymorphism, Genome-wide association study, Locus (genetics), Systemic Sclerosis, Biology, Polymorphism, Single Nucleotide, White People, Genetics, medicine, Humans, GWAS, Genetic Predisposition to Disease, Genomic disorders and inherited multi-system disorders Molecular epidemiology [IGMD 3], Molecular Biology, Genetics (clinical), Genetic association, Scleroderma, Systemic, Association Studies Articles, Receptors, Interleukin-12, General Medicine, Odds ratio, Infection and autoimmunity Auto-immunity, transplantation and immunotherapy [NCMLS 1], United States, Europe, Cohort, Evaluation of complex medical interventions Auto-immunity, transplantation and immunotherapy [NCEBP 2], Medical genetics, Follow-Up Studies, Genome-Wide Association Study
Abstract

A single-nucleotide polymorphism (SNP) at the IL12RB2 locus showed a suggestive association signal in a previously published genome-wide association study (GWAS) in systemic sclerosis (SSc). Aiming to reveal the possible implication of the IL12RB2 gene in SSc, we conducted a follow-up study of this locus in different Caucasian cohorts. We analyzed 10 GWAS-genotyped SNPs in the IL12RB2 region (2309 SSc patients and 5161 controls). We then selected three SNPs (rs3790567, rs3790566 and rs924080) based on their significance level in the GWAS, for follow-up in an independent European cohort comprising 3344 SSc and 3848 controls. The most-associated SNP (rs3790567) was further tested in an independent cohort comprising 597 SSc patients and 1139 controls from the USA. After conditional logistic regression analysis of the GWAS data, we selected rs3790567 [PMH5 1.92 3 10 -5 odds ratio (OR) 5 1.19] as the genetic variant with the firmest independent association observed in the analyzedGWASpeak of association. After the first follow-up phase, only the association of rs3790567 was consistent (PMH5 4.84 3 10 -3OR 5 1.12). The second follow-up phase confirmed this finding (Px2 5 2.82 3 10 -4 OR 5 1.34). After performing overall pooled-analysis of all the cohorts included in the present study, the association found for the rs3790567 SNP in the IL12RB2 gene region reached GWAS-level significant association (PMH5 2.82 3 10 -9 OR 5 1.17). Our data clearly support the IL12RB2 genetic association with SSc, and suggest a relevant role of the interleukin 12 signaling pathway in SSc pathogenesis. © The Author 2011. Published by Oxford University Press. All rights reserved.

Published
2012
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35. Influence of the IL6 Gene in Susceptibility to Systemic Sclerosis

Author

Cenit, M.C., Simeon, C.P., Vonk, M.C., Callejas-Rubio, J.L., Espinosa, G., Carreira, P., Blanco, F.J., Narvaez, J., Tolosa, C., Roman-Ivorra, J.A., Gomez-Garcia, I., Garcia-Hernandez, F.J., Gallego, M., Garcia-Portales, R., Egurbide, M.V., Fonollosa, V., Garcia de la Pena, P., Lopez-Longo, F.J., Gonzalez-Gay, M.A., The Spanish Scleroderma, G., Hesselstrand, R., Riemekasten, G., Witte, T.J.M. de, Voskuyl, A.E., Schuerwegh, A.J., Madhok, R., Fonseca, C., Denton, C., Nordin, A., Palm, O., Laar, J.M. van, Hunzelmann, N., Distler, J.H., Kreuter, A., Herrick, A., Worthington, J., Koeleman, B.P., Radstake, T.R.D.J., Martin, J., Rheumatology, and CCA - Innovative therapy

Subjects
Male, Immunology, Disease, Polymorphism, Single Nucleotide, White People, symbols.namesake, Rheumatology, medicine, Humans, Immunology and Allergy, SNP, Genetic Predisposition to Disease, Allele, Interleukin 6, skin and connective tissue diseases, Autoimmune disease, Scleroderma, Systemic, biology, Interleukin-6, business.industry, medicine.disease, Infection and autoimmunity Auto-immunity, transplantation and immunotherapy [NCMLS 1], Europe, Minor allele frequency, Bonferroni correction, Meta-analysis, Disease Progression, symbols, biology.protein, Evaluation of complex medical interventions Auto-immunity, transplantation and immunotherapy [NCEBP 2], Female, business
Abstract

Objective.Systemic sclerosis (SSc) is a genetically complex autoimmune disease; the genetic component has not been fully defined. Interleukin 6 (IL-6) plays a crucial role in immunity and fibrosis, both key aspects of SSc. We investigated the influence of IL6 gene in the susceptibility and phenotype expression of SSc.Methods.We performed a large metaanalysis including a total of 2749 cases and 3189 controls from 6 white populations (Germany, The Netherlands, Norway, Spain, Sweden, and United Kingdom). Three IL6 single-nucleotide polymorphisms (SNP; rs2069827, rs1800795, and rs2069840) were selected by SNP tagging and genotyped using TaqMan® allele discrimination technology.Results.Individual SNP metaanalysis showed no evidence of association of the 3 IL6 genetic variants with the global disease. Phenotype analyses revealed a significant association between the minor allele of rs2069840 and the limited cutaneous SSc clinical form (Bonferroni p = 0.036, OR 1.14, 95% CI 1.04–1.25). A trend of association between the minor allele of the rs1800795 and the diffuse cutaneous SSc clinical form was also evident (Bonferroni p = 0.072, OR 0.86, 95% CI 0.77–0.96). In the IL6 allelic combination analyses, the GGC allelic combination rs2069827-rs1800795-rs2069840 showed an association with overall SSc (Bonferroni p = 0.016, OR 1.13, 95% CI 1.04–1.23).Conclusion.Our results suggest that the IL6 gene may influence the development of SSc and its progression.

Published
2012
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38. A genome-wide association study follow-up suggests a possible role for PPARG in systemic sclerosis susceptibility

Author

Lopez-Isac, E., Bossini-Castillo, L., Simeon, C.P., Egurbide, M.V., Alegre-Sancho, J.J., Callejas, J.L., Roman-Ivorra, J.A., Freire, M., Beretta, L., Santaniello, A., Airo, P., Lunardi, C., Hunzelmann, N., Riemekasten, G., Witte, T. de, Kreuter, A., Distler, J.H., Schuerwegh, A.J., Vonk, M.C., Voskuyl, A.E., Shiels, P.G., Laar, J.M. van, Fonseca, C., Denton, C., Herrick, A., Worthington, J., Assassi, S., Koeleman, B.P., Mayes, M.D., Radstake, T.R.D.J., Martin, J., et al., Lopez-Isac, E., Bossini-Castillo, L., Simeon, C.P., Egurbide, M.V., Alegre-Sancho, J.J., Callejas, J.L., Roman-Ivorra, J.A., Freire, M., Beretta, L., Santaniello, A., Airo, P., Lunardi, C., Hunzelmann, N., Riemekasten, G., Witte, T. de, Kreuter, A., Distler, J.H., Schuerwegh, A.J., Vonk, M.C., Voskuyl, A.E., Shiels, P.G., Laar, J.M. van, Fonseca, C., Denton, C., Herrick, A., Worthington, J., Assassi, S., Koeleman, B.P., Mayes, M.D., Radstake, T.R.D.J., Martin, J., and et al.

Abstract

Contains fulltext : 137741.pdf (publisher's version ) (Open Access), INTRODUCTION: A recent genome-wide association study (GWAS) comprising a French cohort of systemic sclerosis (SSc) reported several non-HLA single-nucleotide polymorphisms (SNPs) showing a nominal association in the discovery phase. We aimed to identify previously overlooked susceptibility variants by using a follow-up strategy. METHODS: Sixty-six non-HLA SNPs showing a P value <10-4 in the discovery phase of the French SSc GWAS were analyzed in the first step of this study, performing a meta-analysis that combined data from the two published SSc GWASs. A total of 2,921 SSc patients and 6,963 healthy controls were included in this first phase. Two SNPs, PPARG rs310746 and CHRNA9 rs6832151, were selected for genotyping in the replication cohort (1,068 SSc patients and 6,762 healthy controls) based on the results of the first step. Genotyping was performed by using TaqMan SNP genotyping assays. RESULTS: We observed nominal associations for both PPARG rs310746 (PMH = 1.90 x 10-6, OR, 1.28) and CHRNA9 rs6832151 (PMH = 4.30 x 10-6, OR, 1.17) genetic variants with SSc in the first step of our study. In the replication phase, we observed a trend of association for PPARG rs310746 (P value = 0.066; OR, 1.17). The combined overall Mantel-Haenszel meta-analysis of all the cohorts included in the present study revealed that PPARG rs310746 remained associated with SSc with a nominal non-genome-wide significant P value (PMH = 5.00 x 10-7; OR, 1.25). No evidence of association was observed for CHRNA9 rs6832151 either in the replication phase or in the overall pooled analysis. CONCLUSION: Our results suggest a role of PPARG gene in the development of SSc.

Published
2014

39. Multicriteria decision analysis methods with 1000Minds for developing systemic sclerosis classification criteria

Author

Johnson, S.R., Naden, R.P., Fransen, J., Hoogen, F.H.J. van den, Pope, J.E., Baron, M., Tyndall, A., Matucci-Cerinic, M., Denton, C.P., Distler, O., Gabrielli, A., Laar, J.M. van, Mayes, M., Steen, V., Seibold, J.R., Clements, P., Medsger, T.A., Carreira, P.E., Riemekasten, G., Chung, L., Fessler, B.J., Merkel, P.A., Silver, R., Varga, J., Allanore, Y., Mueller-Ladner, U., Vonk, M.C., Walker, U.A., Cappelli, S., Khanna, D., Johnson, S.R., Naden, R.P., Fransen, J., Hoogen, F.H.J. van den, Pope, J.E., Baron, M., Tyndall, A., Matucci-Cerinic, M., Denton, C.P., Distler, O., Gabrielli, A., Laar, J.M. van, Mayes, M., Steen, V., Seibold, J.R., Clements, P., Medsger, T.A., Carreira, P.E., Riemekasten, G., Chung, L., Fessler, B.J., Merkel, P.A., Silver, R., Varga, J., Allanore, Y., Mueller-Ladner, U., Vonk, M.C., Walker, U.A., Cappelli, S., and Khanna, D.

Abstract

Contains fulltext : 137489.pdf (publisher's version ) (Closed access), OBJECTIVES: Classification criteria for systemic sclerosis (SSc) are being developed. The objectives were to develop an instrument for collating case data and evaluate its sensibility; use forced-choice methods to reduce and weight criteria; and explore agreement among experts on the probability that cases were classified as SSc. STUDY DESIGN AND SETTING: A standardized instrument was tested for sensibility. The instrument was applied to 20 cases covering a range of probabilities that each had SSc. Experts rank ordered cases from highest to lowest probability; reduced and weighted the criteria using forced-choice methods; and reranked the cases. Consistency in rankings was evaluated using intraclass correlation coefficients (ICCs). RESULTS: Experts endorsed clarity (83%), comprehensibility (100%), face and content validity (100%). Criteria were weighted (points): finger skin thickening (14-22), fingertip lesions (9-21), friction rubs (21), finger flexion contractures (16), pulmonary fibrosis (14), SSc-related antibodies (15), Raynaud phenomenon (13), calcinosis (12), pulmonary hypertension (11), renal crisis (11), telangiectasia (10), abnormal nailfold capillaries (10), esophageal dilation (7), and puffy fingers (5). The ICC across experts was 0.73 [95% confidence interval (CI): 0.58, 0.86] and improved to 0.80 (95% CI: 0.68, 0.90). CONCLUSIONS: Using a sensible instrument and forced-choice methods, the number of criteria were reduced by 39% (range, 23-14) and weighted. Our methods reflect the rigors of measurement science and serve as a template for developing classification criteria.

Published
2014

40. New insight on the Xq28 association with systemic sclerosis

Author

Carmona, F.D., Cenit, M.C., Diaz-Gallo, L.M., Broen, J.C., Simeon, C.P., Carreira, P.E., Callejas-Rubio, J.L., Fonollosa, V., Lopez-Longo, F.J., Gonzalez-Gay, M.A., Hunzelmann, N., Riemekasten, G., Witte, T. de, Kreuter, A., Distler, J.H., Madhok, R., Shiels, P., Laar, J.M. van, Schuerwegh, A.J., Vonk, M.C., Voskuyl, A.E., Fonseca, C., Denton, C.P., Herrick, A., Worthington, J., Arnett, F.C., Tan, F.K., Assassi, S., Radstake, T.R., Mayes, M.D., Martin, J., Scleroderma, G. Spanish, Carmona, F.D., Cenit, M.C., Diaz-Gallo, L.M., Broen, J.C., Simeon, C.P., Carreira, P.E., Callejas-Rubio, J.L., Fonollosa, V., Lopez-Longo, F.J., Gonzalez-Gay, M.A., Hunzelmann, N., Riemekasten, G., Witte, T. de, Kreuter, A., Distler, J.H., Madhok, R., Shiels, P., Laar, J.M. van, Schuerwegh, A.J., Vonk, M.C., Voskuyl, A.E., Fonseca, C., Denton, C.P., Herrick, A., Worthington, J., Arnett, F.C., Tan, F.K., Assassi, S., Radstake, T.R., Mayes, M.D., Martin, J., and Scleroderma, G. Spanish

Abstract

Item does not contain fulltext, OBJECTIVE: To evaluate whether the systemic sclerosis (SSc)-associated IRAK1 non-synonymous single-nucleotide polymorphism rs1059702 is responsible for the Xq28 association with SSc or whether there are other independent signals in the nearby methyl-CpG-binding protein 2 gene (MECP2). METHODS: We analysed a total of 3065 women with SSc and 2630 unaffected controls from five independent Caucasian cohorts. Four tag single-nucleotide polymorphisms of MECP2 (rs3027935, rs17435, rs5987201 and rs5945175) and the IRAK1 variant rs1059702 were genotyped using TaqMan predesigned assays. A meta-analysis including all cohorts was performed to test the overall effect of these Xq28 polymorphisms on SSc. RESULTS: IRAK1 rs1059702 and MECP2 rs17435 were associated specifically with diffuse cutaneous SSc (PFDR=4.12x10(-3), OR=1.27, 95% CI 1.09 to 1.47, and PFDR=5.26x10(-4), OR=1.30, 95% CI 1.14 to 1.48, respectively), but conditional logistic regression analysis showed that the association of IRAK1 rs1059702 with this subtype was explained by that of MECP2 rs17435. On the other hand, IRAK1 rs1059702 was consistently associated with presence of pulmonary fibrosis (PF), because statistical significance was observed when comparing SSc patients PF+ versus controls (PFDR=0.039, OR=1.30, 95% CI 1.07 to 1.58) and SSc patients PF+ versus SSc patients PF- (p=0.025, OR=1.26, 95% CI 1.03 to 1.55). CONCLUSIONS: Our data clearly suggest the existence of two independent signals within the Xq28 region, one located in IRAK1 related to PF and another in MECP2 related to diffuse cutaneous SSc, indicating that both genes may have an impact on the clinical outcome of the disease.

Published
2013

41. 2013 classification criteria for systemic sclerosis: an American college of rheumatology/European league against rheumatism collaborative initiative

Author

Hoogen, F.H.J. van den, Khanna, D., Fransen, J., Johnson, S.R., Baron, M., Tyndall, A., Matucci-Cerinic, M., Naden, R.P., Medsger, T.A., Carreira, P.E., Riemekasten, G., Clements, P.J., Denton, C.P., Distler, O., Allanore, Y., Furst, D.E., Gabrielli, A., Mayes, M.D., Laar, J.M. van, Seibold, J.R., Czirjak, L., Steen, V.D., Inanc, M., Kowal-Bielecka, O., Müller-Ladner, U., Valentini, G., Veale, D.J., Vonk, M.C., Walker, U.A., Chung, L., Collier, D.H., Csuka, M.E., Fessler, B.J., Guiducci, S., Herrick, A., Hsu, V.M., Jimenez, S., Kahaleh, B., Merkel, P.A., Sierakowski, S., Silver, R.M., Simms, R., Varga, J., Pope, J.E., Hoogen, F.H.J. van den, Khanna, D., Fransen, J., Johnson, S.R., Baron, M., Tyndall, A., Matucci-Cerinic, M., Naden, R.P., Medsger, T.A., Carreira, P.E., Riemekasten, G., Clements, P.J., Denton, C.P., Distler, O., Allanore, Y., Furst, D.E., Gabrielli, A., Mayes, M.D., Laar, J.M. van, Seibold, J.R., Czirjak, L., Steen, V.D., Inanc, M., Kowal-Bielecka, O., Müller-Ladner, U., Valentini, G., Veale, D.J., Vonk, M.C., Walker, U.A., Chung, L., Collier, D.H., Csuka, M.E., Fessler, B.J., Guiducci, S., Herrick, A., Hsu, V.M., Jimenez, S., Kahaleh, B., Merkel, P.A., Sierakowski, S., Silver, R.M., Simms, R., Varga, J., and Pope, J.E.

Abstract

Item does not contain fulltext

Published
2013

42. Confirmation of TNIP1 but not RHOB and PSORS1C1 as systemic sclerosis risk factors in a large independent replication study

Author

Bossini-Castillo, L., Martin, J.E., Broen, J., Simeon, C.P., Beretta, L., Gorlova, O.Y., Vonk, M.C., Ortego-Centeno, N., Espinosa, G., Carreira, P., Garcia de la Pena, P., Oreiro, N., Roman-Ivorra, J.A., Castillo, M.J., Gonzalez-Gay, M.A., Saez-Comet, L., Castellvi, I., Schuerwegh, A.J., Voskuyl, A.E., Hoffmann-Vold, A.M., Hesselstrand, R., Nordin, A., Lunardi, C., Scorza, R., Laar, J.M. van, Shiels, P.G., Herrick, A., Worthington, J., Fonseca, C., Denton, C., Tan, F.K., Arnett, F.C., Assassi, S., Koeleman, B.P., Mayes, M.D., Radstake, T.R.D.J., Martin, J., et al., Bossini-Castillo, L., Martin, J.E., Broen, J., Simeon, C.P., Beretta, L., Gorlova, O.Y., Vonk, M.C., Ortego-Centeno, N., Espinosa, G., Carreira, P., Garcia de la Pena, P., Oreiro, N., Roman-Ivorra, J.A., Castillo, M.J., Gonzalez-Gay, M.A., Saez-Comet, L., Castellvi, I., Schuerwegh, A.J., Voskuyl, A.E., Hoffmann-Vold, A.M., Hesselstrand, R., Nordin, A., Lunardi, C., Scorza, R., Laar, J.M. van, Shiels, P.G., Herrick, A., Worthington, J., Fonseca, C., Denton, C., Tan, F.K., Arnett, F.C., Assassi, S., Koeleman, B.P., Mayes, M.D., Radstake, T.R.D.J., Martin, J., and et al.

Abstract

Item does not contain fulltext, INTRODUCTION: A recent genome-wide association study in European systemic sclerosis (SSc) patients identified three loci (PSORS1C1, TNIP1 and RHOB) as novel genetic risk factors for the disease. The aim of this study was to replicate the previously mentioned findings in a large multicentre independent SSc cohort of Caucasian ancestry. METHODS: 4389 SSc patients and 7611 healthy controls from different European countries and the USA were included in the study. Six single nucleotide polymorphisms (SNP): rs342070, rs13021401 (RHOB), rs2233287, rs4958881, rs3792783 (TNIP1) and rs3130573 (PSORS1C1) were analysed. Overall significance was calculated by pooled analysis of all the cohorts. Haplotype analyses and conditional logistic regression analyses were carried out to explore further the genetic structure of the tested loci. RESULTS: Pooled analyses of all the analysed SNPs in TNIP1 revealed significant association with the whole disease (rs2233287 p(MH)=1.94x10(-4), OR 1.19; rs4958881 p(MH)=3.26x10(-5), OR 1.19; rs3792783 p(MH)=2.16x10(-4), OR 1.19). These associations were maintained in all the subgroups considered. PSORS1C1 comparison showed association with the complete set of patients and all the subsets except for the anti-centromere-positive patients. However, the association was dependent on different HLA class II alleles. The variants in the RHOB gene were not associated with SSc or any of its subsets. CONCLUSIONS: These data confirmed the influence of TNIP1 on an increased susceptibility to SSc and reinforced this locus as a common autoimmunity risk factor.

Published
2013

43. The systemic lupus erythematosus IRF5 risk haplotype is associated with systemic sclerosis

Author

Carmona, F.D., Martin, J.E., Beretta, L., Simeon, C.P., Carreira, P.E., Callejas, J.L., Fernandez-Castro, M., Saez-Comet, L., Beltran, E., Camps, M.T., Egurbide, M.V., Airo, P., Scorza, R., Lunardi, C., Hunzelmann, N., Riemekasten, G., Witte, T. de, Kreuter, A., Distler, J.H., Madhok, R., Shiels, P., Laar, J.M. van, Fonseca, C., Denton, C., Herrick, A., Worthington, J., Schuerwegh, A.J., Vonk, M.C., Voskuyl, A.E., Radstake, T.R.D.J., Martin, J., et al., Carmona, F.D., Martin, J.E., Beretta, L., Simeon, C.P., Carreira, P.E., Callejas, J.L., Fernandez-Castro, M., Saez-Comet, L., Beltran, E., Camps, M.T., Egurbide, M.V., Airo, P., Scorza, R., Lunardi, C., Hunzelmann, N., Riemekasten, G., Witte, T. de, Kreuter, A., Distler, J.H., Madhok, R., Shiels, P., Laar, J.M. van, Fonseca, C., Denton, C., Herrick, A., Worthington, J., Schuerwegh, A.J., Vonk, M.C., Voskuyl, A.E., Radstake, T.R.D.J., Martin, J., and et al.

Abstract

Contains fulltext : 117843.pdf (publisher's version ) (Open Access), Systemic sclerosis (SSc) is a fibrotic autoimmune disease in which the genetic component plays an important role. One of the strongest SSc association signals outside the human leukocyte antigen (HLA) region corresponds to interferon (IFN) regulatory factor 5 (IRF5), a major regulator of the type I IFN pathway. In this study we aimed to evaluate whether three different haplotypic blocks within this locus, which have been shown to alter the protein function influencing systemic lupus erythematosus (SLE) susceptibility, are involved in SSc susceptibility and clinical phenotypes. For that purpose, we genotyped one representative single-nucleotide polymorphism (SNP) of each block (rs10488631, rs2004640, and rs4728142) in a total of 3,361 SSc patients and 4,012 unaffected controls of Caucasian origin from Spain, Germany, The Netherlands, Italy and United Kingdom. A meta-analysis of the allele frequencies was performed to analyse the overall effect of these IRF5 genetic variants on SSc. Allelic combination and dependency tests were also carried out. The three SNPs showed strong associations with the global disease (rs4728142: P = 1.34x10(-8), OR = 1.22, CI 95% = 1.14-1.30; rs2004640: P = 4.60x10(-7), OR = 0.84, CI 95% = 0.78-0.90; rs10488631: P = 7.53x10(-20), OR = 1.63, CI 95% = 1.47-1.81). However, the association of rs2004640 with SSc was not independent of rs4728142 (conditioned P = 0.598). The haplotype containing the risk alleles (rs4728142*A-rs2004640*T-rs10488631*C: P = 9.04x10(-22), OR = 1.75, CI 95% = 1.56-1.97) better explained the observed association (likelihood P-value = 1.48x10(-4)), suggesting an additive effect of the three haplotypic blocks. No statistical significance was observed in the comparisons amongst SSc patients with and without the main clinical characteristics. Our data clearly indicate that the SLE risk haplotype also influences SSc predisposition, and that this association is not sub-phenotype-specific.

Published
2013

44. Implication of IL-2/IL-21 region in systemic sclerosis genetic susceptibility

Author

Diaz-Gallo, L.M., Simeon, C.P., Broen, J.C.A., Ortego-Centeno, N., Beretta, L., Vonk, M.C., Carreira, P.E., Vargas, S., Roman-Ivorra, J.A., Gonzalez-Gay, M.A., Tolosa, C., Lopez-Longo, F.J., Espinosa, G., Vicente, E.F., Hesselstrand, R., Riemekasten, G., Witte, T. de, Distler, J.H., Voskuyl, A.E., Schuerwegh, A.J., Shiels, P.G., Nordin, A., Padyukov, L., Hoffmann-Vold, A.M., Scorza, R., Lunardi, C., Airo, P., Laar, J.M. van, Hunzelmann, N., Gathof, B.S., Kreuter, A., Herrick, A., Worthington, J., Denton, C.P., Zhou, X., Arnett, F.C., Fonseca, C., Koeleman, B.P., Assasi, S., Radstake, T.R.D.J., Mayes, M.D., Martin, J., et al., Diaz-Gallo, L.M., Simeon, C.P., Broen, J.C.A., Ortego-Centeno, N., Beretta, L., Vonk, M.C., Carreira, P.E., Vargas, S., Roman-Ivorra, J.A., Gonzalez-Gay, M.A., Tolosa, C., Lopez-Longo, F.J., Espinosa, G., Vicente, E.F., Hesselstrand, R., Riemekasten, G., Witte, T. de, Distler, J.H., Voskuyl, A.E., Schuerwegh, A.J., Shiels, P.G., Nordin, A., Padyukov, L., Hoffmann-Vold, A.M., Scorza, R., Lunardi, C., Airo, P., Laar, J.M. van, Hunzelmann, N., Gathof, B.S., Kreuter, A., Herrick, A., Worthington, J., Denton, C.P., Zhou, X., Arnett, F.C., Fonseca, C., Koeleman, B.P., Assasi, S., Radstake, T.R.D.J., Mayes, M.D., Martin, J., and et al.

Abstract

Item does not contain fulltext, OBJECTIVE: The interleukin 2 (IL-2) and interleukin 21 (IL-21) locus at chromosome 4q27 has been associated with several autoimmune diseases, and both genes are related to immune system functions. The aim of this study was to evaluate the role of the IL-2/IL-21 locus in systemic sclerosis (SSc). PATIENTS AND METHODS: The case control study included 4493 SSc Caucasian patients and 5856 healthy controls from eight Caucasian populations (Spain, Germany, The Netherlands, USA, Italy, Sweden, UK and Norway). Four single nucleotide polymorphisms (rs2069762, rs6822844, rs6835457 and rs907715) were genotyped using TaqMan allelic discrimination assays. RESULTS: We observed evidence of association of the rs6822844 and rs907715 variants with global SSc (pc=6.6E-4 and pc=7.2E-3, respectively). Similar statistically significant associations were observed for the limited cutaneous form of the disease. The conditional regression analysis suggested that the most likely genetic variation responsible for the association was the rs6822844 polymorphism. Consistently, the rs2069762A-rs6822844T-rs6835457G-rs907715T allelic combination showed evidence of association with SSc and limited cutaneous SSc subtype (pc=1.7E-03 and pc=8E-4, respectively). CONCLUSIONS: These results suggested that the IL-2/IL-21 locus influences the genetic susceptibility to SSc. Moreover, this study provided further support for the IL-2/IL-21 locus as a common genetic factor in autoimmune diseases.

Published
2013

45. A replication study confirms the association of TNFSF4 (OX40L) polymorphisms with systemic sclerosis in a large European cohort

Author

Bossini-Castillo, L., Broen, J.C.A., Simeon, C.P., Beretta, L., Vonk, M.C., Ortego-Centeno, N., Espinosa, G., Carreira, P., Camps, M.T., Navarrete, N., Gonzalez-Escribano, M.F., Vicente-Rabaneda, E., Rodriguez, L., Tolosa, C., Roman-Ivorra, J.A., Gomez-Gracia, I., Garcia-Hernandez, F.J., Castellvi, I., Gallego, M., Fernandez-Nebro, A., Garcia-Portales, R., Egurbide, M.V., Fonollosa, V., Pena, P.G. de la, Pros, A., Gonzalez-Gay, M.A., Hesselstrand, R., Riemekasten, G., Witte, T.J.M. de, Coenen, M.J.H., Koeleman, B.P., Houssiau, F., Smith, V., Keyser, F. de, Westhovens, R., Langhe, E. De, Voskuyl, A.E., Schuerwegh, A.J., Chee, M.M., Madhok, R., Shiels, P., Fonseca, C., Denton, C., Claes, K., Padykov, L., Nordin, A., Palm, O., Lie, B.A., Airo, P., Scorza, R., Laar, J.M. van, Hunzelmann, N., Kreuter, A., Herrick, A., Worthington, J., Radstake, T.R.D.J., Martin, J., Rueda, B., Bossini-Castillo, L., Broen, J.C.A., Simeon, C.P., Beretta, L., Vonk, M.C., Ortego-Centeno, N., Espinosa, G., Carreira, P., Camps, M.T., Navarrete, N., Gonzalez-Escribano, M.F., Vicente-Rabaneda, E., Rodriguez, L., Tolosa, C., Roman-Ivorra, J.A., Gomez-Gracia, I., Garcia-Hernandez, F.J., Castellvi, I., Gallego, M., Fernandez-Nebro, A., Garcia-Portales, R., Egurbide, M.V., Fonollosa, V., Pena, P.G. de la, Pros, A., Gonzalez-Gay, M.A., Hesselstrand, R., Riemekasten, G., Witte, T.J.M. de, Coenen, M.J.H., Koeleman, B.P., Houssiau, F., Smith, V., Keyser, F. de, Westhovens, R., Langhe, E. De, Voskuyl, A.E., Schuerwegh, A.J., Chee, M.M., Madhok, R., Shiels, P., Fonseca, C., Denton, C., Claes, K., Padykov, L., Nordin, A., Palm, O., Lie, B.A., Airo, P., Scorza, R., Laar, J.M. van, Hunzelmann, N., Kreuter, A., Herrick, A., Worthington, J., Radstake, T.R.D.J., Martin, J., and Rueda, B.

Abstract

Contains fulltext : 96595.pdf (publisher's version ) (Closed access), OBJECTIVES: The aim of this study was to confirm the influence of TNFSF4 polymorphisms on systemic sclerosis (SSc) susceptibility and phenotypic features. METHODS: A total of 8 European populations of Caucasian ancestry were included, comprising 3014 patients with SSc and 3125 healthy controls. Four genetic variants of TNFSF4 gene promoter (rs1234314, rs844644, rs844648 and rs12039904) were selected as genetic markers. RESULTS: A pooled analysis revealed the association of rs1234314 and rs12039904 polymorphisms with SSc (OR 1.15, 95% CI 1.02 to 1.31; OR 1.18, 95% CI 1.08 to 1.29, respectively). Significant association of the four tested variants with patients with limited cutaneous SSc (lcSSc) was revealed (rs1234314 OR 1.22, 95% CI 1.07 to 1.38; rs844644 OR 0.91, 95% CI 0.83 to 0.99; rs844648 OR 1.10, 95% CI 1.01 to 1.20 and rs12039904 OR 1.20, 95% CI 1.09 to 1.33). Association of rs1234314, rs844648 and rs12039904 minor alleles with patients positive for anti-centromere antibodies (ACA) remained significant (OR 1.23, 95% CI 1.10 to 1.37; OR 1.12, 95% CI 1.01 to 1.25; OR 1.22, 95% CI 1.07 to 1.38, respectively). Haplotype analysis confirmed a protective haplotype associated with SSc, lcSSc and ACA positive subgroups (OR 0.88, 95% CI 0.82 to 0.96; OR 0.88, 95% CI 0.80 to 0.96; OR 0.86, 95% CI 0.77 to 0.97, respectively) and revealed a new risk haplotype associated with the same groups of patients (OR 1.14, 95% CI 1.03 to 1.26; OR 1.20, 95% CI 1.08 to 1.35; OR 1.23, 95% CI 1.07 to 1.42, respectively). CONCLUSIONS: The data confirm the influence of TNFSF4 polymorphisms in SSc genetic susceptibility, especially in subsets of patients positive for lcSSc and ACA.

Published
2011

46. Confirmation of association of the macrophage migration inhibitory factor gene with systemic sclerosis in a large European population

Author

Bossini-Castillo, L., Simeon, C.P., Beretta, L., Vonk, M.C., Callejas-Rubio, J.L., Espinosa, G., Carreira, P., Camps, M.T., Rodriguez-Rodriguez, L., Rodriguez-Carballeira, M., Garcia-Hernandez, F.J., Lopez-Longo, F.J., Hernandez-Hernandez, V., Saez-Comet, L., Egurbide, M.V., Hesselstrand, R., Nordin, A., Hoffmann-Vold, A.M., Vanthuyne, M., Smith, V., Langhe, E. De, Kreuter, A., Riemekasten, G., Witte, T.J.M. de, Hunzelmann, N., Voskuyl, A.E., Schuerwegh, A.J., Lunardi, C., Airo, P., Scorza, R., Shiels, P., Laar, J.M. van, Fonseca, C., Denton, C., Herrick, A., Worthington, J., Koeleman, B.P., Rueda, B., Radstake, T.R.D.J., Martin, J., Bossini-Castillo, L., Simeon, C.P., Beretta, L., Vonk, M.C., Callejas-Rubio, J.L., Espinosa, G., Carreira, P., Camps, M.T., Rodriguez-Rodriguez, L., Rodriguez-Carballeira, M., Garcia-Hernandez, F.J., Lopez-Longo, F.J., Hernandez-Hernandez, V., Saez-Comet, L., Egurbide, M.V., Hesselstrand, R., Nordin, A., Hoffmann-Vold, A.M., Vanthuyne, M., Smith, V., Langhe, E. De, Kreuter, A., Riemekasten, G., Witte, T.J.M. de, Hunzelmann, N., Voskuyl, A.E., Schuerwegh, A.J., Lunardi, C., Airo, P., Scorza, R., Shiels, P., Laar, J.M. van, Fonseca, C., Denton, C., Herrick, A., Worthington, J., Koeleman, B.P., Rueda, B., Radstake, T.R.D.J., and Martin, J.

Abstract

Contains fulltext : 96758.pdf (publisher's version ) (Closed access), Objectives. The aim of this study was to confirm the implication of macrophage migration inhibitory factor (MIF) gene in SSc susceptibility or clinical phenotypes in a large European population. Methods. A total of 3800 SSc patients and 4282 healthy controls of white Caucasian ancestry from eight different European countries were included in the study. The MIF -173 single nucleotide polymorphism (SNP) was selected as genetic marker and genotyped using Taqman 5' allelic discrimination assay. Results. The MIF -173 SNP showed association with SSc [P = 0.04, odds ratio (OR) = 1.10, 95% CI 1.00, 1.19]. Analysis of the MIF -173 polymorphism according to SSc clinical phenotype revealed that the frequency of the -173*C allele was significantly higher in the dcSSc group compared with controls (P = 5.30E-03, OR = 1.21, 95% CI 1.07, 1.38). Conversely, the frequency of the MIF -173*C allele was significantly underrepresented in the lcSSc group compared with dcSSc patients, supporting previous findings [(P = 0.04, OR = 0.86, 95% CI 0.75, 0.99); meta-analysis including previous results (P = 0.005, OR = 0.83, 95% CI 0.73, 0.94)]. Conclusion. Our results confirm the role of MIF -173 promoter polymorphism in SSc, and provide evidence of a strong association with the dcSSc subgroup of patients. Hence, the MIF -173 variant is confirmed as a promising clinical phenotype genetic marker.

Published
2011

47. Association of a non-synonymous functional variant of the ITGAM gene with systemic sclerosis

Author

Carmona, F.D., Simeon, C.P., Beretta, L., Carreira, P., Vonk, M.C., Rios-Fernandez, R., Espinosa, G., Navarrete, N., Vicente-Rabaneda, E., Rodriguez-Rodriguez, L., Tolosa, C., Garcia-Hernandez, F.J., Castellvi, I., Egurbide, M.V., Fonollosa, V., Gonzalez-Gay, M.A., Rodriguez-Carballeira, M., Diaz-Gonzalez, F., Saez-Comet, L., Hesselstrand, R., Riemekasten, G., Witte, T.J.M. de, Voskuyl, A.E., Schuerwegh, A.J., Madhok, R., Shiels, P., Fonseca, C., Denton, C., Nordin, A., Palm, O., Hoffmann-Vold, A.M., Airo, P., Scorza, R., Lunardi, C., Laar, J.M. van, Hunzelmann, N., Kreuter, A., Herrick, A., Worthington, J., Koeleman, B.P., Radstake, T.R.D.J., Martin, J., Carmona, F.D., Simeon, C.P., Beretta, L., Carreira, P., Vonk, M.C., Rios-Fernandez, R., Espinosa, G., Navarrete, N., Vicente-Rabaneda, E., Rodriguez-Rodriguez, L., Tolosa, C., Garcia-Hernandez, F.J., Castellvi, I., Egurbide, M.V., Fonollosa, V., Gonzalez-Gay, M.A., Rodriguez-Carballeira, M., Diaz-Gonzalez, F., Saez-Comet, L., Hesselstrand, R., Riemekasten, G., Witte, T.J.M. de, Voskuyl, A.E., Schuerwegh, A.J., Madhok, R., Shiels, P., Fonseca, C., Denton, C., Nordin, A., Palm, O., Hoffmann-Vold, A.M., Airo, P., Scorza, R., Lunardi, C., Laar, J.M. van, Hunzelmann, N., Kreuter, A., Herrick, A., Worthington, J., Koeleman, B.P., Radstake, T.R.D.J., and Martin, J.

Abstract

Contains fulltext : 97656.pdf (publisher's version ) (Closed access)

Published
2011

48. Characteristics of joint involvement and relationships with systemic inflammation in systemic sclerosis: results from the EULAR Scleroderma Trial and Research Group (EUSTAR) database.

Author

Avouac, J., Walker, U., Tyndall, A., Kahan, A., Matucci-Cerinic, M., Allanore, Y., Miniati, I., Muller, A., Iannone, F., Distler, O., Becvar, R., Sierakowsky, S., Kowal-Bielecka, O., Coelho, P.C., Cabane, J., Cutolo, M., Shoenfeld, Y., Valentini, G., Rovensky, J., Riemekasten, G., Vlachoyiannopoulos, P.G., Caporali, R., Jiri, S., Inanc, M., Zimmermann Gorska, I., Carreira, P., Novak, S., Czirjak, L., Oliveira Ramos, F., Jendro, M., Chizzolini, C., Kucharz, E.J., Richter, J., Cozzi, F., Rozman, B., Mallia, C.M., Gabrielli, A., Farge, D., Kiener, H., Schoffel, D., Airo, P., Wollheim, F., Martinovic, D., Trotta, F., Jablonska, S., Reich, K., Bombardieri, S., Siakka, P., Pellerito, R., Bambara, L.M., Morovic-Vergles, J., Denton, C., Hinrichs, R., Hoogen, F.H.J. van den, Damjanov, N., Kotter, I., Ortiz, V., Heitmann, S., Krasowska, D., Seidel, M., Hasler, P., Laar, J.M. van, Kaltwasser, J.P., Foeldvari, I., Juan Mas, A., Bajocchi, G., Wislowska, M., Pereira Da Silva, J.A., Jacobsen, S., Worm, M.H.J.B., Graniger, W., Kuhn, A., Stankovic, A., Cossutta, R., Majdan, M., Damjanovska Rajcevska, L., Tikly, M., Nasonov, E.L., Steinbrink, K., Herrick, A., Muller-Ladner, U., Dinc, A., Scorza, R., Sondergaard, K., Indiveri, F., Nielsen, H., Szekanecz, Z., Silver, R.M., Antivalle, M., Espinosa, I.B., Garcia de la Pena Lefebvre, P., Midtvedt, O., Launay, D. de, Valesini, F., Tuvik, P., Vonk, M.C., et al., Avouac, J., Walker, U., Tyndall, A., Kahan, A., Matucci-Cerinic, M., Allanore, Y., Miniati, I., Muller, A., Iannone, F., Distler, O., Becvar, R., Sierakowsky, S., Kowal-Bielecka, O., Coelho, P.C., Cabane, J., Cutolo, M., Shoenfeld, Y., Valentini, G., Rovensky, J., Riemekasten, G., Vlachoyiannopoulos, P.G., Caporali, R., Jiri, S., Inanc, M., Zimmermann Gorska, I., Carreira, P., Novak, S., Czirjak, L., Oliveira Ramos, F., Jendro, M., Chizzolini, C., Kucharz, E.J., Richter, J., Cozzi, F., Rozman, B., Mallia, C.M., Gabrielli, A., Farge, D., Kiener, H., Schoffel, D., Airo, P., Wollheim, F., Martinovic, D., Trotta, F., Jablonska, S., Reich, K., Bombardieri, S., Siakka, P., Pellerito, R., Bambara, L.M., Morovic-Vergles, J., Denton, C., Hinrichs, R., Hoogen, F.H.J. van den, Damjanov, N., Kotter, I., Ortiz, V., Heitmann, S., Krasowska, D., Seidel, M., Hasler, P., Laar, J.M. van, Kaltwasser, J.P., Foeldvari, I., Juan Mas, A., Bajocchi, G., Wislowska, M., Pereira Da Silva, J.A., Jacobsen, S., Worm, M.H.J.B., Graniger, W., Kuhn, A., Stankovic, A., Cossutta, R., Majdan, M., Damjanovska Rajcevska, L., Tikly, M., Nasonov, E.L., Steinbrink, K., Herrick, A., Muller-Ladner, U., Dinc, A., Scorza, R., Sondergaard, K., Indiveri, F., Nielsen, H., Szekanecz, Z., Silver, R.M., Antivalle, M., Espinosa, I.B., Garcia de la Pena Lefebvre, P., Midtvedt, O., Launay, D. de, Valesini, F., Tuvik, P., Vonk, M.C., and et al.

Abstract

Contains fulltext : 87872.pdf (publisher's version ) (Closed access)

Published
2010

49. Systemic sclerosis and its pulmonary complications in The Netherlands: an epidemiological study.

Author

Vonk, M.C., Broers, B., Heijdra, Y.F., Ton, E., Snijder, R., Dijk, A.P.J. van, Laar, J.M. van, Bootsma, H.J., Hal, P.T. van, Hoogen, F.H.J. van den, Daele, P.L. van, Vonk, M.C., Broers, B., Heijdra, Y.F., Ton, E., Snijder, R., Dijk, A.P.J. van, Laar, J.M. van, Bootsma, H.J., Hal, P.T. van, Hoogen, F.H.J. van den, and Daele, P.L. van

Abstract

Contains fulltext : 81439.pdf (publisher's version ) (Closed access), The prevalence and incidence of systemic sclerosis (SSc) in The Netherlands is unknown. The same holds true for its leading causes of death: pulmonary fibrosis and pulmonary arterial hypertension (PAH), for which effective treatment options have recently become available. OBJECTIVE: To establish the prevalence and incidence of SSc and its pulmonary complications. METHODS: Detailed information on patients in the POEMAS registry, "Pulmonary Hypertension Screening, a Multidisciplinary Approach in Scleroderma", consisting of 819 patients, was combined with a nationwide questionnaire. RESULTS: By combining the two sources the prevalence of SSc was found to be 8.9 per 100 000 adults. The incidence was 0.77 patients per 100 000 per year. PAH was diagnosed in 9.9% of SSc patients. The prevalence of interstitial lung disease in SSc varied from 19% to 47% depending on the definition used. CONCLUSION: This study clarifies the epidemiology of SSc in The Netherlands and confirms the frequent occurrence of pulmonary complications, based on 654 cases. This can and will be studied further in the ongoing POEMAS study.

Published
2009

50. Long-term follow-up results after autologous haematopoietic stem cell transplantation for severe systemic sclerosis.

Author

Vonk, M.C., Marjanovic, Z., Hoogen, F.H.J. van den, Zohar, S., Schattenberg, A.V.M.B., Fibbe, W.E., Larghero, J., Gluckman, E., Preijers, F.W.M.B., Dijk, A.P.J. van, Bax, J.J., Roblot, P., Riel, P.L.C.M. van, Laar, J.M. van, Farge, D., Vonk, M.C., Marjanovic, Z., Hoogen, F.H.J. van den, Zohar, S., Schattenberg, A.V.M.B., Fibbe, W.E., Larghero, J., Gluckman, E., Preijers, F.W.M.B., Dijk, A.P.J. van, Bax, J.J., Roblot, P., Riel, P.L.C.M. van, Laar, J.M. van, and Farge, D.

Abstract

Contains fulltext : 69053schattenberg.pdf (publisher's version ) (Closed access), OBJECTIVE: Systemic sclerosis (SSc) is a generalised autoimmune disease, causing morbidity and a reduced life expectancy, especially in patients with rapidly progressive diffuse cutaneous SSc. As no proven treatment exists, autologous haematopoietic stem cell transplantation (HSCT) is employed as a new therapeutic strategy in patients with a poor prognosis. This study reports the effects on survival, skin and major organ function of HSCT in patients with severe diffuse cutaneous SSc. PATIENTS AND METHODS: A total of 26 patients were evaluated. Peripheral blood stem cells were collected using cyclophosphamide (4 g/m2) and rHu G-CSF (5 to 10 microg/kg/day) and were reinfused after positive CD34+ selection. For conditioning, cyclophosphamide 200 mg/kg was used. RESULTS: After a median follow-up of 5.3 (1-7.5) years, 81% (n = 21/26) of the patients demonstrated a clinically beneficial response. The Kaplan-Meier estimated survival at 5 years was 96.2% (95% CI 89-100%) and at 7 years 84.8% (95% CI 70.2-100%) and event-free survival, defined as survival without mortality, relapse or progression of SSc, resulting in major organ dysfunction was 64.3% (95% CI 47.9-86%) at 5 years and 57.1% (95% CI 39.3-83%) at 7 years. CONCLUSION: This study confirms that autologous HSCT in selected patients with severe diffuse cutaneous SSc results in sustained improvement of skin thickening and stabilisation of organ function up to 7 years after transplantation.

Published
2008

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