Your search keyword '"de Vries, Niek"' showing total 17 results

1. Sensitive B-cell receptor repertoire analysis shows repopulation correlates with clinical response to rituximab in rheumatoid arthritis

Author

Pollastro, Sabrina, Musters, Anne, Balzaretti, Giulia, Niewold, Ilse, van Schaik, Barbera, Hässler, Signe, Verhoef, Catharina M., Pallardy, Marc, van Kampen, Antoine, Mariette, Xavier, and de Vries, Niek

Published

2024

2. Genome-wide association analysis of anti-TNF drug response in patients with rheumatoid arthritis

Author

Mirkov, Maša Umiċeviċ, Cui, Jing, Vermeulen, Sita H, Stahl, Eli A, Toonen, Erik JM, Makkinje, Remco R, Lee, Annette T, Huizinga, Tom WJ, Allaart, Renee, Barton, Anne, Mariette, Xavier, Miceli, Corinne Richard, Criswell, Lindsey A, Tak, Paul P, de Vries, Niek, Saevarsdottir, Saedis, Padyukov, Leonid, Bridges, S Louis, van Schaardenburg, Dirk-Jan, Jansen, Tim L, Dutmer, Ellen AJ, van de Laar, Mart AFJ, Barrera, Pilar, Radstake, Timothy RDJ, van Riel, Piet LCM, Scheffer, Hans, Franke, Barbara, Brunner, Han G, Plenge, Robert M, Gregersen, Peter K, Guchelaar, Henk-Jan, and Coenen, Marieke JH

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Arthritis, Rheumatoid Arthritis, Genetics, Autoimmune Disease, Human Genome, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Adalimumab, Antibodies, Monoclonal, Antibodies, Monoclonal, Humanized, Antirheumatic Agents, Arthritis, Rheumatoid, DNA Mutational Analysis, Drug Resistance, Etanercept, Female, Gene Expression Regulation, Genetic Markers, Genome-Wide Association Study, Humans, Immunoglobulin G, Infliximab, Male, Polymorphism, Single Nucleotide, Receptors, Tumor Necrosis Factor, Registries, Tumor Necrosis Factor-alpha, Anti-TNF, Gene Polymorphism, Pharmacogenetics, Public Health and Health Services, Arthritis & Rheumatology, Clinical sciences

Abstract

BackgroundTreatment strategies blocking tumour necrosis factor (anti-TNF) have proven very successful in patients with rheumatoid arthritis (RA). However, a significant subset of patients does not respond for unknown reasons. Currently, there are no means of identifying these patients before treatment. This study was aimed at identifying genetic factors predicting anti-TNF treatment outcome in patients with RA using a genome-wide association approach.MethodsWe conducted a multistage, genome-wide association study with a primary analysis of 2 557 253 single-nucleotide polymorphisms (SNPs) in 882 patients with RA receiving anti-TNF therapy included through the Dutch Rheumatoid Arthritis Monitoring (DREAM) registry and the database of Apotheekzorg. Linear regression analysis of changes in the Disease Activity Score in 28 joints after 14 weeks of treatment was performed using an additive model. Markers with p

Published

2013

3. Latitude gradient influences the age of onset of rheumatoid arthritis: a worldwide survey

Author

Ramos-Remus, Cesar, Ramirez-Gomez, Andrea, Brambila-Barba, Victor, Barajas-Ochoa, Aldo, Castillo-Ortiz, Jose D., Adebajo, Adewale O., Espinoza, Luis R., Aceves-Avila, Francisco J., Sánchez-González, Jorge M., Boudersa, Nadia, Slimani, Samy, Ladjouze-Rezig, Aicha, Diaz, Mónica P., Kirmayr, Karin I., Asnal, Cecilia A., Catoggio, Luis J., Citera, Gustavo, Casado, Gustavo C., Alvarez, Analia P., Pisoni, Cecilia N., Benavente, Emilio, Lopez-Cabanillas, Adriana, Baez, Roberto M., Pons-Estel, Bernardo A., Sacnún, Mónica P., Cavallasca, Javier A., Paniego, Raúl H., Proudman, Susanna M., Thomas, Ranjeny, Major, Gabor, Mathers, David M., Schrieber, Leslie, Haq, Syed A., Islam, Nazrul, Dessein, Patrick H., von Muhlen, Carlos A., Bianchi, Washington A., da R. Castelar-Pinheiro, Geraldo, Feldman-Pollak, Daniel, Cossermelli, Waldenise, Bonfiglioli, Karina R., Giorgi, Rina D., Zabsonre-Tiendrebeogo, Wendlassida J., Russell, Anthony S., Olaru, Lilia, Karsh, Jacob, Fuentealba, Carlos, Aguilera, Sergio, Castro-Esparza, Irene H., Burgos, Paula I., Neira, Oscar, Li, Zhan-guo, Tam, Lai-Shan, Mok, Mo Y., Medina, Yimy F., Moreno-Alvarez, Mario J., Zúñiga-Vera, Andrés E., Vera, Claudia, Quezada, Ivonne, Moreno, Iván M., Calapaqui, Wendy, El-Mardenly, Ghada, Salama, M. Salah, Ragab, Gaafar, Hadidi, Tahsin, Gado, Kamel, Leirisalo-Repo, Marjatta, Tuompo, Riitta, Koivuniemi, Riitta, Berenbaum, Francis, Allanore, Yannick, Constantin, Arnaud, Buttgereit, Frank, Schulze-Koops, Hendrik, Liz, Myriam, Dey, Dzifa, Alonzo-Borjas, Hugo D., Santiago-Pastelín, Carlos B., Cuéllar-Cruz, Víctor, Dharmanand, Balebail G., Yathish, G. C., Akerkar, Shashank M., Malaviya, Anand N., Ahmadzadeh, Arman, Hasunuma, Tomoko, Owino, Benard O., Pacheco-Tena, César, Frausto-Arenas, Aaron, De la Madrid-Cernas, Adrián A., Cardona-Cabrera, Román, Centeno-Valadez, Juan D., Rodríguez-Torres, Isaura M., Vaidya, Binit, Gupta, Arun K., Harrison, Andrew A., Grainger, Rebecca, Nwankwo, Henry M., Diamantopoulos, Andreas P., Mæland, Elisabeth, Besada, Emilio, Gorriz, Luis, Duarte, Margarita, Albrecht, Maria T. Romero-de, Cabrera-Villalba, Sonia, Segami, María I., García-Poma, Augusto, Pérez-Medina, Wilkerson, Ramos, María P., Navarra, Sandra V., Racaza, Geraldine Z., Penserga, Ester G., Manapat-Reyes, Bernadette H., Dianongco, Maria L., Lichauco, Juan J., Torralba, Tito P., Al-Emadi, Samar, Hammoudeh, Mohammed, Botchkova, Anna G., AlSaeedi, Sabri H., Almoallim, Hani, Al-Arfaj, Hussein F., Koh, Wei H., Leung, Ying Y., Whitelaw, David A., Hodkinson, Bridget, García-Miguel, Javier, Duro, Juan C., Andreu, José L., Martin-Mola, Emilio, Ahijón-Lana, María, Finckh, Axel, Alpízar-Rodríguez, Deshiré, Osiri, Manathip, Kasitanon, Nuntana, Louthrenoo, Worawit, de Vries, Niek, van Denderen, Christiaan, Gerritsen, Martjin, van Vollenhoven, Ronald F., Jansen, Tim L., van Riel, Piet, Núñez-Sotelo, Concepción M., Villegas-Morales, Sol, and GEO-RA Group

Published

2017

4. Increased Frequency of CD4+ Follicular Helper T and CD8+ Follicular T Cells in Human Lymph Node Biopsies during the Earliest Stages of Rheumatoid Arthritis

Author

Anang, Dornatien Chuo, Ramwadhdoebe, Tamara H, Hähnlein, Janine S, Van Kuijk, Bo, Smits, Noortje, Van Lienden, Krijn P, Maas, Mario, Gerlag, Daniëlle M, Tak, Paul P, De Vries, Niek, Van Baarsen, Lisa GM, Clinical Immunology and Rheumatology, AII - Inflammatory diseases, Graduate School, AGEM - Digestive immunity, Radiology and Nuclear Medicine, AMS - Rehabilitation & Development, AMS - Sports, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Experimental Immunology, Anang, Dornatien Chuo [0000-0001-5454-2639], Tak, Paul P [0000-0002-3532-5409], van Baarsen, Lisa GM [0000-0003-3346-8921], Apollo - University of Cambridge Repository, and Radiology and nuclear medicine

Subjects

Arthritis, Rheumatoid, Lymphoid Tissue, Biopsy, T lymphocytes, Humans, T-Lymphocytes, Helper-Inducer, General Medicine, CD8-Positive T-Lymphocytes, Rheumatoid arthritis, rheumatoid arthritis, lymph nodes, B lymphocytes, follicular T helper cells, Follicular T helper cells, Lymph nodes

Abstract

Follicular T helper cells (Tfh cells) provide key B-cell help and are essential in germinal center formation and (auto) antibody generation. To gain more insight into their role during the earliest phase of rheumatoid arthritis (RA), we analyzed their frequencies, phenotypes, and cytokine profiles in peripheral blood and lymph node biopsies of healthy controls (HCs), autoantibody-positive individuals at risk for developing RA (RA-risk individuals), and early RA patients. Subsequently, we confirmed their presence in lymph nodes and synovial tissue of RA patients using immunofluorescence microscopy. In the blood, the frequency of Tfh cells did not differ between study groups. In lymphoid and synovial tissues, Tfh cells were localized in B-cell areas, and their frequency correlated with the frequency of CD19+ B cells. Compared to lymphoid tissues of healthy controls, those of RA patients and RA-risk individuals showed more CD19+ B cells, CD4+CXCR5+ follicular helper T cells, and CD8+CXCR5+ follicular T cells. These Tfh cells produced less IL-21 upon ex vivo stimulation. These findings suggest that Tfh cells may present a novel rationale for therapeutic targeting during the preclinical stage of RA to prevent further disease progression.

Published

2022

5. In rheumatoid arthritis inflamed joints share dominant patientspecific B-cell clones.

Author

Musters, Anne, Balzaretti, Giulia, van Schaik, Barbera D. C., Jongejan, Aldo, van der Weele, Linda, Tas, Sander W., van Kampen, Antoine H. C., and de Vries, Niek

Subjects

RHEUMATOID arthritis, SYNOVIAL fluid, ANTIGEN receptors, B cells, INFLAMMATION

Abstract

Background: In patients with rheumatoid arthritis (RA) different joints were shown to share the same dominant T-cell clones, suggesting shared characteristics of the inflammatory process and indicating that strategies to selectively target the antigen receptor might be feasible. Since T- and Blymphocytes closely interact in adaptive responses, we analysed to what extent different joints also share dominant B-cell clones. Methods: In 11 RA patients, quantitative B-cell receptor (BCR) repertoire analysis was performed in simultaneously obtained samples from inflamed synovial tissue (ST) from distinct locations within one joint, from multiple joints, from synovial fluid (SF) and peripheral blood (PB). Results: ST biopsies from different locations in the same joint showed clear overlap in the top-25 dominant BCR clones (16.7%, SD 12.5), in the same range as the overlap between ST and SF in the same joint (8.0%, SD 8.8) and the overlap between ST-ST between different joints (9.1%, SD 8.2), but clearly higher than the overlap between ST and PB (1.7%, SD 2.4; p<0.05) and SF and PB (2.7%, SD 4.1; p<0.05). Interestingly, these figures were substantially lower than the overlap observed in previous T-cell clonality studies. Conclusions: We conclude that in RA BCR clonal responses may be more localized than TCR clonal responses, pointing to antigen-selective influx, proliferation and/or maturation of B-cells. B lineage cells in the SF may adequately represent the dominant BCR clones of the ST, which is in contrast to T-cells. Collectively, the presence of shared B- and especially T-cells in different joints from the same patient suggests that approaches might be feasible that aim to develop antigen-receptor specific targeting of lymphocyte clones in RA as an alternative tomore generalized immunosuppressive strategies. [ABSTRACT FROM AUTHOR]

Published

2022

6. Restoration of Default Blood Monocyte-Derived Macrophage Polarization With Adalimumab But Not Etanercept in Rheumatoid Arthritis.

Author

Paoletti, Audrey, Ly, Bineta, Bitoun, Samuel, Nocturne, Gaëtane, Rivière, Elodie, Manson, Jessica J., Matucci, Andrea, Pallardy, Marc, De Vries, Niek, and Mariette, Xavier

Subjects

RHEUMATOID arthritis, TUMOR necrosis factors, MACROPHAGES, ADALIMUMAB, ETANERCEPT

Abstract

Introduction: We previously reported a specific defect of rheumatoid arthritis (RA) monocyte polarization to anti-inflammatory M2-like macrophages related to increased miR-155 expression in all RA patients except those receiving adalimumab (ADA). In this longitudinal study, we examined whether different tumor necrosis factor inhibitors were able to restore monocyte polarization to M2-like macrophages and their effect on the transcriptomic signature. Methods: M2-like polarization induced by human serum AB was studied in 7 healthy donors and 20 RA patients included in the ABIRA cohort before and 3 months after starting ADA or etanercept (ETA). The differential gene expression of M2- and M1-related transcripts was studied in macrophage-derived monocytes after differentiation. Results: At baseline, RA monocytes showed a defect of polarization to M2-like macrophages as compared with healthy donor monocytes, which was negatively correlated with disease activity. M2-like polarization from circulating monocytes was restored only with ADA and not ETA treatment. The transcriptomic signature demonstrated downregulation of M2-related transcripts and upregulation of M1-related transcripts in active RA. In patients receiving ADA, the transcriptomic signature of M2-related transcripts was restored. Conclusion: This longitudinal study demonstrates that ADA but not ETA is able to restore the M2-like polarization of monocytes that is defective in RA. [ABSTRACT FROM AUTHOR]

Published

2022

7. Non-response to rituximab therapy in rheumatoid arthritis is associated with incomplete disruption of the B cell receptor repertoire.

Author

Pollastro, Sabrina, Klarenbeek, Paul L., Doorenspleet, Marieke E., van Schaik, Barbera D. C., Esveldt, Rebecca E. E., Thurlings, Rogier M., Boumans, Maria J. H., Gerlag, Danielle M., Tak, Paul P., Vos, Koen, Baas, Frank, van Kampen, Antoine H. C., and de Vries, Niek

Abstract

Objective: To gain more insight into the dynamics of lymphocyte depletion and develop new predictors of clinical response to rituximab in rheumatoid arthritis (RA).Methods: RNA-based next-generation sequencing was used to analyse the B cell receptor (BCR) repertoire in peripheral blood and synovial tissue samples collected from 24 seropositive patients with RA treated with rituximab. Clonal expansion, mutation load and clonal overlap were assessed in samples collected before, at week 4 and at week 16 or 24 after treatment and correlated to the patients' clinical response.Results: After 4 weeks of rituximab-induced B cell depletion, the peripheral blood BCR repertoire of treated patients consisted of fewer, more dominant and more mutated BCR clones. No significant changes in the synovial tissue BCR repertoire were detected until week 16 post-treatment, when a reduced clonal overlap with baseline and an increased mutation load were observed. In patients who were non-responders at month 3 (n=5) using the European League Against Rheumatism response criteria, peripheral blood samples taken at week 4 after rituximab treatment showed more dominant clones compared with moderate responders (n=9) (median (IQR): 36 (27-52) vs 18 (16-26); p<0.01) and more clonal overlap with the baseline (median (IQR): 5% (2%-20%) vs 0% (0%-0%); p≤0.01).Conclusion: Significant changes in BCR clonality are observed in peripheral blood of patients 4 weeks after rituximab treatment, while changes in synovial tissue were observed at later time points. Incomplete depletion of the dominant baseline peripheral blood BCR repertoire in the first month of treatment might predict clinical non-response at 3 months. [ABSTRACT FROM AUTHOR]

Published

2019

8. Association of response to TNF inhibitors in rheumatoid arthritis with quantitative trait loci for and CD39.

Author

Spiliopoulou, Athina, Colombo, Marco, Plant, Darren, Nair, Nisha, Jing Cui, Coenen, Marieke J. H., Ikari, Katsunori, Yamanaka, Hisashi, Saevarsdottir, Saedis, Padyukov, Leonid, Bridges, Louis, Kimberly, Robert P., Okada, Yukinori, van Riel, Piet L. C. M., Wolbink, Gertjan, van der Horst-Bruinsma, Irene E., de Vries, Niek, Tak, Paul P., Ohmura, Koichiro, and Canhão, Helena

Abstract

Objectives: We sought to investigate whether genetic effects on response to TNF inhibitors (TNFi) in rheumatoid arthritis (RA) could be localised by considering known genetic susceptibility loci for relevant traits and to evaluate the usefulness of these genetic loci for stratifying drug response.Methods: We studied the relation of TNFi response, quantified by change in swollen joint counts ( Δ SJC) and erythrocyte sedimentation rate ( Δ ESR) with locus-specific scores constructed from genome-wide assocation study summary statistics in 2938 genotyped individuals: 37 scores for RA; scores for 19 immune cell traits; scores for expression or methylation of 93 genes with previously reported associations between transcript level and drug response. Multivariate associations were evaluated in penalised regression models by cross-validation.Results: We detected a statistically significant association between Δ SJC and the RA score at the CD40 locus (p=0.0004) and an inverse association between Δ SJC and the score for expression of CD39 on CD4 T cells (p=0.00005). A previously reported association between CD39 expression on regulatory T cells and response to methotrexate was in the opposite direction. In stratified analysis by concomitant methotrexate treatment, the inverse association was stronger in the combination therapy group and dissipated in the TNFi monotherapy group. Overall, ability to predict TNFi response from genotypic scores was limited, with models explaining less than 1% of phenotypic variance.Conclusions: The association with the CD39 trait is difficult to interpret because patients with RA are often prescribed TNFi after failing to respond to methotrexate. The CD39 and CD40 pathways could be relevant for targeting drug therapy. [ABSTRACT FROM AUTHOR]

Published

2019

9. Dominant B cell receptor clones in peripheral blood predict onset of arthritis in individuals at risk for rheumatoid arthritis.

Author

Tak, Paul P., Doorenspleet, Marieke E., de Hair, Maria J. H., Klarenbeek, Paul L., van Beers-Tas, Marian H., van Kampen, Antoine H. C., van Schaardenburg, Dirkjan, Gerlag, Danielle M., Baas, Frank, and de Vries, Niek

Subjects

AUTOANTIBODY analysis, AUTOANTIBODIES, CELLS, COMPARATIVE studies, JOINTS (Anatomy), LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, RESEARCH, RHEUMATOID arthritis, EVALUATION research, RELATIVE medical risk, PREDICTIVE tests

Abstract

Background: The onset of seropositive rheumatoid arthritis (RA) is preceded by the presence of specific autoantibodies in the absence of synovial inflammation. Only a subset of these at-risk individuals will develop clinical disease. This impedes efforts to implement early interventions that may prevent onset of clinically manifest disease. Here we analyse whether clonal changes in the B cell receptor (BCR) repertoire can reliably predict onset of signs and symptoms.Methods: In a prospective cohort study in 21 individuals at risk for RA based on the presence of autoantibodies, the BCR repertoire of paired peripheral blood and synovial tissue samples was analysed using next-generation BCR sequencing. BCR clones that were expanded beyond 0.5% of the total repertoire were labelled dominant. The relative risk (RR) for onset of arthritis was assessed using the presence of ≥5 dominant BCR clones as cut-off. Findings in peripheral blood were validated in an independent prospective cohort of 50 at-risk individuals. Based on the test cohort, individuals in the validation cohort were considered positive if peripheral blood at study entry showed ≥5 dominant BCR clones.Findings: Both in the test and validation cohort, the presence of ≥5 dominant BCR clones in peripheral blood was significantly associated with arthritis development after follow-up (validation cohort RR 6.3, 95% CI 2.7 to 15, p<1×10-4). Even when adjusted for a recently described clinical prediction rule the association remained intact (RR 5.0, 95% CI 1.2 to 20, p=0.024). When individuals developed arthritis, dominant BCR clones disappeared from peripheral blood and appeared in synovial tissue, suggesting a direct role of these clones in disease pathogenesis.Interpretation: Dominant BCR clones in peripheral blood predict onset of clinical signs and symptoms of RA in at-risk individuals with high accuracy. Our data suggest that during onset of RA these clones shift from peripheral blood to the target tissue. [ABSTRACT FROM AUTHOR]

Published

2017

10. A Novel HLA-DRB1*10:01-Restricted T Cell Epitope From Citrullinated Type II Collagen Relevant to Rheumatoid Arthritis.

Author

Chemin, Karine, Pollastro, Sabrina, James, Eddie, Ge, Changrong, Albrecht, Inka, Herrath, Jessica, Gerstner, Christina, Tandre, Karolina, Sampaio Rizzi, Thais, Rönnblom, Lars, Catrina, Anca, Holmdahl, Rikard, Klareskog, Lars, de Vries, Niek, and Malmström, Vivianne

Subjects

ANTIGEN analysis, CELL culture, COLLAGEN diseases, IMMUNOCHEMISTRY, PEPTIDES, RESEARCH funding, RHEUMATOID arthritis, STATISTICS, T cells, T-test (Statistics), DATA analysis, DATA analysis software, DESCRIPTIVE statistics, SEQUENCE analysis, IN vitro studies

Abstract

Objective Antibodies against citrullinated type II collagen (Cit-CII) are common in the sera and synovial fluid of patients with rheumatoid arthritis (RA); however, the known T cell epitope of CII is not dependent on citrullination. The aim of this study was to identify and functionally characterize the Cit-CII-restricted T cell epitopes that are relevant to RA. Methods Peripheral blood mononuclear cells (PBMCs) from HLA-DRB1*10:01-positive patients with RA and healthy donors were stimulated in vitro with candidate CII peptides. CD154 up-regulation was measured as a marker of antigen-specific activation, and anti-HLA-DR-blocking experiments confirmed HLA restriction. Cytokine production was measured using a Luminex technique. Direct peptide-binding assays using HLA-DRB1*10:01 and HLA-DRB1*04:01 monomeric proteins were performed. The T cell receptor (TCR) β-chain of CD154-enriched antigen-specific T cells was analyzed using high-throughput sequencing. Results A novel Cit-CII peptide was identified based on its ability to activate CD4+ T cells from HLA-DRB1*10:01-positive individuals. When stimulated in vitro, Cit-CII autoreactive T cells produced proinflammatory cytokines. Cit-CII311-325 bound (with low affinity) to HLA-DRB1*10:01 but not to HLA-DRB1*04:01, while the native form was unable to bind either protein. In addition, highly expanded clones were identified in the TCRβ repertoire of Cit-CII311-325-stimulated PBMCs. Conclusion These results illustrate the ability of the citrullination process to create T cell epitopes from CII, a cartilage-restricted protein that is relevant to RA pathogenesis. The exclusive binding of Cit-CII311-325 to HLA-DRB1*10:01 suggests that recognition of citrullinated epitopes might vary between individuals carrying different RA-associated HLA-DR molecules. [ABSTRACT FROM AUTHOR]

Published

2016

11. Rheumatoid Arthritis Risk Allele PTPRC Is Also Associated With Response to Anti-Tumor Necrosis Factor α Therapy.

Author

Jing Cui, Saevarsdottir, Saedis, Thomson, Brian, Padyukov, Leonid, van der Helm-van Mil, Annette H. M., Nititham, Joanne, Hughes, Laura B., de Vries, Niek, Raychaudhuri, Soumya, Alfredsson, Lars, Askling, Johan, Wedrén, Sara, Bo Ding, Guiducci, Candace, Wolbink, Gert Jan, Crusius, J. Bart A., van der Horst-Bruinsma, Irene E., Herenius, Marieke, Weinblatt, Michael E., and Shadick, Nancy A.

Subjects

GENES, RHEUMATOID arthritis, TUMOR necrosis factors, GENETIC polymorphisms, RHEUMATOID factor, AUTOANTIBODIES, AGE, HUMAN sexuality, THERAPEUTICS

Abstract

The article presents a study which examined the response of rheumatoid arthritis risk allele PTPRC to anti-tumor necrosis factor (TNF) alpha therapy. According to the authors, there was strong statistical evidence favoring the association of PTPRC single-nucleotide polymorphism with response to anti-TNF-alpha therapy in patients who were seropositive for either rheumatoid factor and anti-citrullinated protein autoantibodies. They explain that age, sex and drugs were analyzed as correlates of treatment response.

Published

2010

12. The Germinal Center Milieu in Rheumatoid Arthritis: The Immunological Drummer or Dancer?

Author

Anang, Dornatien C., Balzaretti, Giulia, van Kampen, Antoine, de Vries, Niek, and Klarenbeek, Paul L.

Subjects

GERMINAL centers, RHEUMATOID arthritis, ANTIBODY formation, PATHOLOGICAL physiology, AUTOANTIBODIES, B cells

Abstract

Rheumatoid Arthritis (RA) is a chronic autoimmune disease characterized by joint inflammation, affecting approximately 1% of the general population. To alleviate symptoms and ameliorate joint damage, chronic use of immunosuppressives is needed. However, these treatments are only partially effective and may lead to unwanted side effects. Therefore, a more profound understanding of the pathophysiology might lead to more effective therapies, or better still, a cure. The presence of autoantibodies in RA indicates that B cells might have a pivotal role in the disease. This concept is further supported by the fact that a diverse antibody response to various arthritis-related epitopes is associated with arthritis development. In this context, attention has focused in recent years on the role of Germinal Centers (GCs) in RA. Since GCs act as the main anatomic location of somatic hypermutations, and, thus, contributing to the diversity and specificity of (auto) antibodies, it has been speculated that defects in germinal center reactions might be crucial in the initiation and maintenance of auto-immune events. In this paper, we discuss current evidence that various processes within GCs can result in the aberrant production of B cells that possess autoreactive properties and might result in the production of RA related autoantibodies. Secondly, we discuss various (pre-)clinical studies that have targeted various GC processes as novel therapies for RA treatment. [ABSTRACT FROM AUTHOR]

Published

2021

13. New susceptibility locus for rheumatoid arthritis suggested by a genome-wide linkage study.

Author

Cornelis, Francois, Faure, Sabine, Martinez, Maria, Prud'Homme, Jean-Francois, Fritz, Pierre, Dib, Colette, Alves, Helena, Barrera, Pilar, De Vries, Niek, Balsa, Alejandro, Pascual-Salcedo, Dora, Maenaut, Kristin, Westhovens, Rene, Migliorini, Paola, Tran, Tuyet-Hoa, Delaye, Arnaud, Prince, Nathalie, Lefevre, Caroline, Thomas, Gaelle, and Poirier, Murielle

Subjects

RHEUMATOID arthritis, LYMPHOCYTES, ANTIGENS

Abstract

Reports on a study which identified additional rheumatoid arthritis (RA) loci. Association of RA in families with autoimmune diseases; Susceptibility of the human lymphocyte antigen to the locus; Methodology used to conduct the study; Results of the study.

Published

1998

14. Integration of Sequence Data from a Consanguineous Family with Genetic Data from an Outbred Population Identifies PLB1 as a Candidate Rheumatoid Arthritis Risk Gene

Author

Okada, Yukinori, Diogo, Dorothee, Greenberg, Jeffrey D., Mouassess, Faten, Achkar, Walid A. L., Fulton, Robert S., Denny, Joshua C., Gupta, Namrata, Mirel, Daniel, Gabriel, Stacy, Li, Gang, Kremer, Joel M., Pappas, Dimitrios A., Carroll, Robert J., Eyler, Anne E., Trynka, Gosia, Stahl, Eli A., Cui, Jing, Saxena, Richa, Coenen, Marieke J. H., Guchelaar, Henk-Jan, Huizinga, Tom W. J., Dieudé, Philippe, Mariette, Xavier, Barton, Anne, Canhão, Helena, Fonseca, João E., de Vries, Niek, Tak, Paul P., Moreland, Larry W., Bridges, S. Louis, Miceli-Richard, Corinne, Choi, Hyon K., Kamatani, Yoichiro, Galan, Pilar, Lathrop, Mark, Raj, Towfique, De Jager, Philip L., Raychaudhuri, Soumya, Worthington, Jane, Padyukov, Leonid, Klareskog, Lars, Siminovitch, Katherine A., Gregersen, Peter K., Mardis, Elaine R., Arayssi, Thurayya, Kazkaz, Layla A., and Plenge, Robert M.

Subjects

Biology, Computational Biology, Genomics, Genome Analysis Tools, Genome Scans, Genome Sequencing, Molecular Genetics, Gene Identification and Analysis, Genetics, Population Genetics, Genetic Polymorphism, Genetic Screens, Genetics of Disease, Human Genetics, Population Biology, Medicine, Clinical Immunology, Autoimmune Diseases, Rheumatoid Arthritis, Epidemiology, Disease Mapping

Abstract

Integrating genetic data from families with highly penetrant forms of disease together with genetic data from outbred populations represents a promising strategy to uncover the complete frequency spectrum of risk alleles for complex traits such as rheumatoid arthritis (RA). Here, we demonstrate that rare, low-frequency and common alleles at one gene locus, phospholipase B1 (PLB1), might contribute to risk of RA in a 4-generation consanguineous pedigree (Middle Eastern ancestry) and also in unrelated individuals from the general population (European ancestry). Through identity-by-descent (IBD) mapping and whole-exome sequencing, we identified a non-synonymous c.2263G>C (p.G755R) mutation at the PLB1 gene on 2q23, which significantly co-segregated with RA in family members with a dominant mode of inheritance (P = 0.009). We further evaluated PLB1 variants and risk of RA using a GWAS meta-analysis of 8,875 RA cases and 29,367 controls of European ancestry. We identified significant contributions of two independent non-coding variants near PLB1 with risk of RA (rs116018341 [MAF = 0.042] and rs116541814 [MAF = 0.021], combined P = 3.2×10−6). Finally, we performed deep exon sequencing of PLB1 in 1,088 RA cases and 1,088 controls (European ancestry), and identified suggestive dispersion of rare protein-coding variant frequencies between cases and controls (P = 0.049 for C-alpha test and P = 0.055 for SKAT). Together, these data suggest that PLB1 is a candidate risk gene for RA. Future studies to characterize the full spectrum of genetic risk in the PLB1 genetic locus are warranted.

Published

2014

15. Reply.

Author

Chemin, Karine, Albrecht, Inka, Pollastro, Sabrina, de Vries, Niek, Holmdahl, Rikard, and Malmström, Vivianne

Subjects

ALLELES, ANTIGENS, IMMUNOLOGY technique, RESEARCH methodology, PEPTIDES, RHEUMATOID arthritis

Abstract

A response from the authors of the article "A Novel HLA-DRB1*10:01-restricted T cell epitope from citrullinated type II collagen relevant to rheumatoid arthritis" that was published in the previous issue is presented.

Published

2016

16. Effects of B-cell directed therapy on the preclinical stage of rheumatoid arthritis: the PRAIRI study.

Author

Gerlag, Danielle M, Safy, Mary, Maijer, Karen I, Tang, Man Wai, Tas, Sander W, Starmans-Kool, Mirian J F, van Tubergen, Astrid, Janssen, Matthijs, de Hair, Maria, Hansson, Monika, de Vries, Niek, Zwinderman, Aeilko H, and Tak, Paul P

Abstract

Objectives: We explored the effects of B-cell directed therapy in subjects at risk of developing autoantibodypositive rheumatoid arthritis (RA), who never experienced inflammatory arthritis before, and explored biomarkers predictive of arthritis development.Methods: Individuals positive for both anti-citrullinated peptide antibodies and rheumatoid factor but without arthritis were included in a randomised, double-blind, placebo-controlled study to receive a single infusion of 1000 mg rituximab or placebo.Results: Eighty-one individuals received treatment and were followed up for a mean of 29.0 (0-54) months, during which 30/81 (37%) individuals developed arthritis. The observed risk of developing arthritis in the placebo-treated group was 40%, which was decreased by 55% (HR 0.45, 95% CI 0.154 to 1.322) in the rituximab-treated group at 12 months. Rituximab treatment caused a delay in arthritis development of 12 months compared with placebo treatment at the point when 25% of the subjects had developed arthritis (p<0.0001). Erythrocyte sedimentation rate and the presence of anti-citrullinated α-enolase peptide 1 at baseline were significant predictors of arthritis development.Conclusions: A single infusion of 1000 mg rituximab significantly delays the development of arthritis in subjects at risk of developing RA, providing evidence for the pathogenetic role of B cells in the earliest, prearthritis stage of autoantibody positive RA. [ABSTRACT FROM AUTHOR]

Published

2018

17. Crowdsourcing genetic prediction of clinical utility in the Rheumatoid Arthritis Responder Challenge.

Author

Plenge, Robert M, Greenberg, Jeffrey D, Mangravite, Lara M, Derry, Jonathan M J, Stahl, Eli A, Coenen, Marieke J H, Barton, Anne, Padyukov, Leonid, Klareskog, Lars, Gregersen, Peter K, Mariette, Xavier, Moreland, Larry W, Bridges, S Louis, de Vries, Niek, Huizinga, Tom W J, Guchelaar, Henk-Jan, Friend, Stephen H, and Stolovitzky, Gustavo

Subjects

GENETIC research, AUTOIMMUNE diseases, RHEUMATOID arthritis

Abstract

A letter to the editor is presented in response to an article related to challenge to develop genetic predictors of response to immunosuppressive therapy in a common autoimmune disease, rheumatoid arthritis (RA).

Published

2013