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5. 14 Medisch-immunologische diagnostiek

Author

Langerak, A.W., van der Velden, V.H.J., van der Burg, M., Dik, W.A., Schreurs, M.W.J., Benner, R., editor, Kraal, G., editor, van Dissel, J.T., editor, and van Lier, R.A.W., editor

Published
2016
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6. Serum cytokine levels are associated with tumor progression during FOLFIRINOX chemotherapy and overall survival in pancreatic cancer patients

Author

Sijde, F. van der, Dik, W.A., Mustafa, D.A.M., Vietsch, E.E., Besselink, M.G., Debets, R., Koerkamp, B.G., Haberkorn, B.C.M., Homs, M.Y.V., Janssen, Q.P., Luelmo, S.A.C., Mekenkamp, L.J.M., Oostvogels, A.A.M., Nijenhuis, M.A.W.S.T., Wilmink, J.W., Eijck, C.H.J. van, Surgery, Immunology, Pathology, Medical Oncology, CCA - Cancer Treatment and Quality of Life, Amsterdam Gastroenterology Endocrinology Metabolism, Oncology, and CCA - Cancer biology and immunology

Subjects
Interleukin-7, pancreatic cancer, Immunology, Interleukin-18, Leucovorin, treatment response, Irinotecan, Oxaliplatin, Pancreatic Neoplasms, Interleukin 1 Receptor Antagonist Protein, IL-1RA, SDG 3 - Good Health and Well-being, Antineoplastic Combined Chemotherapy Protocols, cytokine, Cytokines, Humans, biomarker, Immunology and Allergy, Fluorouracil, Chemokine CCL4, Carcinoma, Pancreatic Ductal
Abstract

BackgroundBiomarkers predicting treatment response may be used to stratify patients with pancreatic ductal adenocarcinoma (PDAC) for available therapies. The aim of this study was to evaluate the association of circulating cytokines with FOLFIRINOX response and with overall survival (OS).MethodsSerum samples were collected before start and after the first cycle of FOLFIRINOX from patients with PDAC (n=83) of all disease stages. Overall, 34 circulating cytokines were analyzed with a multiplex immunoassay. In addition, changes in peripheral blood immune cell counts were determined by flow cytometry to correlate with differences in cytokine levels. Chemotherapy response was determined by CT scans with the RECIST 1.1 criteria, as disease control (n=64) or progressive disease (n=19) within eight cycles of FOLFIRINOX.ResultsPatients with high serum IL-1RA concentrations after one cycle of chemotherapy were less likely to have tumor progression during FOLFIRINOX (OR 0.25,P=0.040). Increase of circulating IL-1RA concentrations correlated with increase of total, classical (CD14+CD16-), and non-classical monocytes (CD14-CD16+), and dendritic cells. In multivariable cox regression, including the variables chemotherapy response outcome and baseline CA19-9 level, serum concentrations of IL-7 (HR 2.14,P=0.010), IL-18 (HR 2.00,P=0.020), and MIP-1β (HR 0.51,P=0.025) after one cycle of FOLFIRINOX showed correlations with OS.ConclusionsCirculating IL-1RA, IL-7, IL-18, and MIP-1β concentrations are biomarkers associated with FOLFIRINOX response in PDAC patients, suggesting an important role for specific immune cells in chemotherapy response and PDAC progression. Cytokine-based treatment might improve patient outcome and should be evaluated in future studies.

Published
2022

7. Hemostasis Proteins in Invasive Meningococcal and Nonmeningococcal Infections: A Prospective Multicenter Study

Author

Hagedoorn, N.N., Boeddha, N.P., Kohlfuerst, D.S., Anderson, S., Carrol, E.D., Agapow, P., Flier, M. van der, Hazelzet, J., Herberg, J., Kuijpers, T., Levin, M., Martinon-Torres, F., Rijswijk, A. van, Schlapbach, L.J., Vermont, C., Zenz, W., Dik, W.A., Driessen, G., Emonts, M., Hagedoorn, N.N., Boeddha, N.P., Kohlfuerst, D.S., Anderson, S., Carrol, E.D., Agapow, P., Flier, M. van der, Hazelzet, J., Herberg, J., Kuijpers, T., Levin, M., Martinon-Torres, F., Rijswijk, A. van, Schlapbach, L.J., Vermont, C., Zenz, W., Dik, W.A., Driessen, G., and Emonts, M.

Abstract

Item does not contain fulltext, OBJECTIVES: We aimed to describe the variation of hemostasis proteins in children with bacterial infections due to different pathogens ( Neisseria meningitidis, Streptococcus pneumoniae, Staphylococcus aureus , and group A streptococcus [GAS]) and to study hemostasis proteins in relation to mortality. DESIGN: Preplanned analysis in prospective cohort study. SETTING: Hospitals in five European countries (Austria, The Netherlands, Spain, Switzerland, and the United Kingdom). PATIENTS: Admitted children (2012-2016) with community-acquired infections due to meningococci ( n = 83), pneumococci ( n = 64), S. aureus (n = 50), and GAS ( n = 44) with available serum samples collected less than 48 hours after admission. INTERVENTIONS: None. MEASUREMENTS AND MAIN RESULTS: Fibronectin, plasminogen activator inhibitor type 1 (PAI-1), thrombomodulin, and a disintegrin and metalloproteinase with a thrombospondin type 1 motif, member 13 (ADAMTS-13) were measured in serum in 2019-2020. Additionally, von Willebrand factor, protein C, protein S, and factor IX were measured in citrate plasma available from a subset of patients. Outcome measures included in-hospital mortality and disease severity (need for ventilation/inotropes, Pediatric Index of Mortality score).Of 241 children, 21 (8.7%) died and 177 (73.5%) were admitted to PICU. Mortality rate was similar for the pathogen groups. Levels of fibronectin and thrombomodulin differed for the different pathogens ( p < 0.05). Fibronectin levels were lower in GAS infections than in S. pneumoniae and S. aureus infections but did not differ from meningococcal infections. Thrombomodulin levels in meningococcal infections were higher than in S. aureus and pneumococcal infections. Overall, the area under the curve for mortality was 0.81 (95% CI, 0.70-0.92) for thrombomodulin and 0.78 (95% CI, 0.69-0.88) for ADAMTS-13. The association of each hemostasis protein did not vary across pathogens for any of the outcome measures. CONCLUSIONS: Hemostati

Published
2022

9. Parents' Perspectives and Societal Acceptance of Implementation of Newborn Screening for SCID in the Netherlands

Author

Blom, M, Bredius, R.G., Jansen, M.E., Weijman, G., Kemper, E.A., Vermont, C.L., Hollink, I., Dik, W.A., Montfrans, J.M., Gijn, M.E. van, Henriet, S.S., Aerde, K.J. van, Koole, W., Lankester, A.C., Dekkers, E., Schielen, P., Vries, M.C. de, Henneman, L., Burg, M. van der, Blom, M, Bredius, R.G., Jansen, M.E., Weijman, G., Kemper, E.A., Vermont, C.L., Hollink, I., Dik, W.A., Montfrans, J.M., Gijn, M.E. van, Henriet, S.S., Aerde, K.J. van, Koole, W., Lankester, A.C., Dekkers, E., Schielen, P., Vries, M.C. de, Henneman, L., and Burg, M. van der

Abstract

Contains fulltext : 231539.pdf (Publisher’s version ) (Open Access), PURPOSE: While neonatal bloodspot screening (NBS) for severe combined immunodeficiency (SCID) has been introduced more than a decade ago, implementation in NBS programs remains challenging in many countries. Even if high-quality test methods and follow-up care are available, public uptake and parental acceptance are not guaranteed. The aim of this study was to describe the parental perspective on NBS for SCID in the context of an implementation pilot. Psychosocial aspects have never been studied before for NBS for SCID and are important for societal acceptance, a major criterion when introducing new disorders in NBS programs. METHODS: To evaluate the perspective of parents, interviews were conducted with parents of newborns with abnormal SCID screening results (N = 17). In addition, questionnaires about NBS for SCID were sent to 2000 parents of healthy newborns who either participated or declined participation in the SONNET-study that screened 140,593 newborns for SCID. RESULTS: Support for NBS for SCID was expressed by the majority of parents in questionnaires from both a public health perspective and a personal perspective. Parents emphasized the emotional impact of an abnormal screening result in interviews. (Long-term) stress and anxiety can be experienced during and after referral indicating the importance of uniform follow-up protocols and adequate information provision. CONCLUSION: The perspective of parents has led to several recommendations for NBS programs that are considering screening for SCID or other disorders. A close partnership of NBS programs' stakeholders, immunologists, geneticists, and pediatricians-immunologists in different countries is required for moving towards universal SCID screening for all infants.

Published
2021

10. Soluble Interleukin-2 Receptor Is a Promising Serum Biomarker for Granulomatous Disease in Common Variable Immune Deficiency

Author

van Stigt, A.C. (Astrid C.), Dalm, V.A.S.H. (Virgil), Nagtzaam, N.M. (Nicole), van Rijswijk, D.A. (Damian A.), Barendregt, B.H. (Barbara), van Hagen, P.M. (P. Martin), IJspeert, H. (Hanna), Dik, W.A. (Willem), van Stigt, A.C. (Astrid C.), Dalm, V.A.S.H. (Virgil), Nagtzaam, N.M. (Nicole), van Rijswijk, D.A. (Damian A.), Barendregt, B.H. (Barbara), van Hagen, P.M. (P. Martin), IJspeert, H. (Hanna), and Dik, W.A. (Willem)

Published
2021
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11. Detectable A Disintegrin and Metalloproteinase With Thrombospondin Motifs-1 in Serum Is Associated With Adverse Outcome in Pediatric Sepsis

Author

Boeddha, N.P., Driessen, G.J., Hagedoorn, N.N., Kohlfuerst, D.S., Hoggart, C.J., Rijswijk, A.L. van, Ekinci, E., Priem, D., Schlapbach, L.J., Herberg, J.A., Groot, R. de, Anderson, S.T., Fink, C.G., Carrol, E.D., Flier, M. van der, Martinón-Torres, F., Levin, M., Leebeek, F.W.G., Zenz, W., Maat, M.P. de, Hazelzet, Jan A., Emonts, M., Dik, W.A., Boeddha, N.P., Driessen, G.J., Hagedoorn, N.N., Kohlfuerst, D.S., Hoggart, C.J., Rijswijk, A.L. van, Ekinci, E., Priem, D., Schlapbach, L.J., Herberg, J.A., Groot, R. de, Anderson, S.T., Fink, C.G., Carrol, E.D., Flier, M. van der, Martinón-Torres, F., Levin, M., Leebeek, F.W.G., Zenz, W., Maat, M.P. de, Hazelzet, Jan A., Emonts, M., and Dik, W.A.

Abstract

Contains fulltext : 241374.pdf (Publisher’s version ) (Open Access), IMPORTANCE: A Disintegrin and Metalloproteinase with Thrombospondin Motifs-1 is hypothesized to play a role in the pathogenesis of invasive infection, but studies in sepsis are lacking. OBJECTIVES: To study A Disintegrin and Metalloproteinase with Thrombospondin Motifs-1 protein level in pediatric sepsis and to study the association with outcome. DESIGN: Data from two prospective cohort studies. SETTING AND PARTICIPANTS: Cohort 1 is from a single-center study involving children admitted to PICU with meningococcal sepsis (samples obtained at three time points). Cohort 2 includes patients from a multicenter study involving children admitted to the hospital with invasive bacterial infections of differing etiologies (samples obtained within 48 hr after hospital admission). MAIN OUTCOMES AND MEASURES: Primary outcome measure was mortality. Secondary outcome measures were PICU-free days at day 28 and hospital length of stay. RESULTS: In cohort 1 (n = 59), nonsurvivors more frequently had A Disintegrin and Metalloproteinase with Thrombospondin Motifs-1 levels above the detection limit than survivors at admission to PICU (8/11 [73%] and 6/23 [26%], respectively; p = 0.02) and at t = 24 hours (2/3 [67%] and 3/37 [8%], respectively; p = 0.04). In cohort 2 (n = 240), A Disintegrin and Metalloproteinase with Thrombospondin Motifs-1 levels in patients within 48 hours after hospital admission were more frequently above the detection limit than in healthy controls (110/240 [46%] and 14/64 [22%], respectively; p = 0.001). Nonsurvivors more often had detectable A Disintegrin and Metalloproteinase with Thrombospondin Motifs-1 levels than survivors (16/21 [76%] and 94/219 [43%], respectively; p = 0.003), which was mostly attributable to patients with Neisseria meningitidis. CONCLUSIONS AND RELEVANCE: In children with bacterial infection, detection of A Disintegrin and Metalloproteinase with Thrombospondin Motifs-1 within 48 hours after hospital admission is associated with death, part

Published
2021

13. Extensive longitudinal immune profiling reveals sustained innate immune activaton in COVID-19 patients with unfavorable outcome

Author

Schrijver, B., Assmann, J.L.J.C., van Gammeren, A.J., Vermeulen, R.C.H., Portengen, L., Heukels, P., Langerak, A.W., Dik, W.A., van der Velden, V.H.J., Ermens, T.A.A.M., IRAS OH Epidemiology Chemical Agents, and dIRAS RA-2

Subjects
SARS-CoV-2, COVID-19
Abstract

COVID-19 differs substantially between individuals, ranging from mild to severe or even fatal. Heterogeneity in the immune response against SARS-COV-2 likely contributes to this. Therefore, we explored the temporal dynamics of key cellular and soluble mediators of innate and adaptive immune activation in relation to COVID-19 severity and progression. Forty-four patients with a PCR-proven diagnosis of COVID-19 were included. Extensive cellular (leukocytes and T-lymphocyte subsets) and serological immune profiling (cytokines, soluble cell surface molecules, and SARS-CoV-2 antibodies) was performed at hospital admission and every 3-4 days during hospitalization. Measurements and disease outcome were compared between patients with an unfavorable (IC admission and/or death) and favorable (all others) outcome. Patients with an unfavorable outcome had higher leukocyte numbers at baseline, mostly due to increased neutrophils, whereas lymphocyte and monocyte numbers were reduced. CRP, IL-6, CCL2, CXCL10, and GM-CSF levels were higher at baseline in the unfavorable group, whereas IL-7 levels were lower. SARS-CoV-2 antibodies were more frequently absent in the unfavorable group. Longitudinal analysis revealed delayed kinetics of activated CD4 and CD8 T-lymphocyte subsets in the unfavorable group. Furthermore, whereas CRP, IL-6, CXCL10, andGM-CSF declinedin the favorable group, these cytokines declined with delayed kinetics, remained increased, or even increased further in the unfavorable group. Our data indicate a state of increased innate immune activation in COVID19-patients with an unfavorable outcome at hospital admission, which remained over time, as compared with patients with a favorable outcome.

Published
2020

14. Increased group 2 innate lymphoid cells in peripheral blood of adults with mastocytosis

Author

Ploeg, E.K. (Esmee) van der, Hermans, M.A.W. (Maud A.W.), Velden, V.H.J. (Vincent) van der, Dik, W.A. (Willem), Daele, P.L.A. (Paul) van, Stadhouders, R. (Ralph), Ploeg, E.K. (Esmee) van der, Hermans, M.A.W. (Maud A.W.), Velden, V.H.J. (Vincent) van der, Dik, W.A. (Willem), Daele, P.L.A. (Paul) van, and Stadhouders, R. (Ralph)

Abstract

Background: Systemic mastocytosis is a hematological disease in which aberrant mast cells accumulate because of gain-of-function mutations in the KIT receptor. Group 2 innate lymphoid cells (ILC2s) are effector cells of type 2 immune responses that also express KIT and colocalize with mast cells at barrier tissue sites. In mouse models, mast cell-ILC2 crosstalk can drive local inflammation. However, a possible role for ILC2s in the pathophysiology of mastocytosis remains unexplored. Objective: We sought to characterize circulating ILC2s in a clinically diverse cohort of patients with mastocytosis. Methods: We included 21 adults with systemic mastocytosis and 18 healthy controls. Peripheral blood ILC2 abundance and phenotype were analyzed by flow cytometry and correlated to clinical characteristics, including the presence of the D816V KIT mutation. Results: ILC2 levels were significantly higher in D816V+ patients with mastocytosis compared with D816V− patients or healthy controls. We observed increased proportions of KIT+ ILC2s among patients with mastocytosis, regardless of D816V status. Patients with skin involvement and itch showed the highest levels of ILC2s, which was independent from atopy or serum tryptase levels. Allele-specific quantitative PCR showed that the vast majority of ILC2s did not carry the D816V mutation. Conclusions: Our findings suggest a role for ILC2s and pathogenic ILC2-mast cell crosstalk in mastocytosis. We hypothesize that a high cutaneous D816V+ m

Published
2020
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15. Inverse correlation between serum complement component C1q levels and whole blood type-1 interferon signature in active tuberculosis and QuantiFERON-positive uveitis: implications for diagnosis

Author

Schrijver, B. (Benjamin), Dijkstra, D.J., Borggreven, N.V., Nora, R.L., Huijser, E., Versnel, M.A. (Marjan), Hagen, P.M. (Martin) van, Joosten, S.A., Trouw, L.A. (L.), Dik, W.A. (Willem), Schrijver, B. (Benjamin), Dijkstra, D.J., Borggreven, N.V., Nora, R.L., Huijser, E., Versnel, M.A. (Marjan), Hagen, P.M. (Martin) van, Joosten, S.A., Trouw, L.A. (L.), and Dik, W.A. (Willem)

Abstract

Objectives To examine the relation between serum C1q levels and blood type‐1 interferon signature (type‐1 IFN signature) in active pulmonary tuberculosis (APTB) and to determine whether combined measurement of serum C1q and type‐1 IFN signature may add to the diagnosis of QuantiFERON‐positive (QFT+) patients with uveitis of unknown cause. Methods C1q was determined (ELISA) in serum from two distinct Indonesian cohorts, and in total, APTB (n = 72), QFT+ uveitis of unknown aetiology (n = 58), QFT− uveitis (n = 51) patients and healthy controls (HC; n = 73) were included. The type‐1 IFN signature scores were previously determined. Results Serum C1q was higher in APTB than HC (P < 0.001). APTB patients with uveitis had higher serum C1q than APTB patients without uveitis (P = 0.0207). Serum C1q correlated inversely with type‐1 IFN signature scores in APTB (P = 0.0036, r2 = 0.3526), revealing that these biomarkers for active TB disease can be mutually exclusive. Stratification of QFT+ patients with uveitis of unknown cause, by serum C1q and type‐1 IFN signature, yielded four groups with different likelihood of suffering from active TB uveitis. Conclusion Serum C1q is elevated in APTB, es

Published
2020
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16. The Impact of Obesity and Lifestyle on the Immune System and Susceptibility to Infections Such as COVID-19

Author

de Frel, D.L. (Daan L.), Atsma, D.E. (Douwe), Pijl, H. (Hanno), Seidell, J.C. (Jaap), Leenen, P.J.M. (Pieter), Dik, W.A. (Willem), van Rossum, E.F.C. (Elisabeth F. C.), de Frel, D.L. (Daan L.), Atsma, D.E. (Douwe), Pijl, H. (Hanno), Seidell, J.C. (Jaap), Leenen, P.J.M. (Pieter), Dik, W.A. (Willem), and van Rossum, E.F.C. (Elisabeth F. C.)

Abstract

Background: COVID-19 is a global challenge to healthcare. Obesity is common in patients with COVID-19 and seems to aggravate disease prognosis. In this review we explore the link between obesity, chronic disease, lifes

Published
2020
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18. Are Patients at Risk for Recurrent Disease Activity After Switching From Remicade® to Remsima®? An Observational Study

Author

Xue, L. (Laixi), Van Bilsen, K. (Kiki), Schreurs, M.W.J. (Marco), Velthoven, M.E. (Mirjam ) van, Missotten, T. (Tom), Thiadens, A.A.H.J. (Alberta), Kuijpers, R.W.A.M. (Robert), Biezen, P. (Paula) van, Dalm, V.A.S.H. (Virgil), Laar, J.A.M. (Jan) van, Hermans, M.A.W. (Maud A.W.), Dik, W.A. (Willem), Daele, P.L.A. (Paul) van, van Hagen, P.M. (P. M.), Xue, L. (Laixi), Van Bilsen, K. (Kiki), Schreurs, M.W.J. (Marco), Velthoven, M.E. (Mirjam ) van, Missotten, T. (Tom), Thiadens, A.A.H.J. (Alberta), Kuijpers, R.W.A.M. (Robert), Biezen, P. (Paula) van, Dalm, V.A.S.H. (Virgil), Laar, J.A.M. (Jan) van, Hermans, M.A.W. (Maud A.W.), Dik, W.A. (Willem), Daele, P.L.A. (Paul) van, and van Hagen, P.M. (P. M.)

Abstract

Background: Since the late ‘90s, infliximab (Remicade®) is being used successfully to treat patients with several non-infectious immune mediated inflammatory diseases (IMIDs). In recent years, infliximab biosimilars, including Remsima® were introduced in clinical practice. Aim: To investigate the interchangeability of Remicade® (originator infliximab) and its biosimilar Remsima® in patients with rare immune-mediated inflammatory diseases (IMIDs). Methods: This two-phased prospective open label observational study was designed to monitor the transition from Remicade® to Remsima® in patients with rare IMIDs. All included patients were followed during the first 2 years. The primary endpoint was the demonstration of non-difference in quality of life and therapeutic efficacy, as measured by parameters including a safety monitoring program, physicians perception of disease activity (PPDA) and patient self-reported outcomes (PSROs). Secondary outcomes included routine blood analysis, pre-infusion serum drug concentration values and anti-drug antibody formation. Results: Forty eight patients treated with Remicade® were switched to Remsima® in June-July 2016 and subsequently monitored during the first 2 years. The group consisted of patients with sarcoidosis (n = 17), Behçet's disease (n = 12), non-infectious uveitis (n = 11), and other diagnoses (n = 8). There were no significant differences in PPDA, PSROs, clinical and laboratory assessments and pre-infusion serum drug concentrations between the groups. De novo anti-drug antibodies were observed in two patients. Seven patients with sarcoidosis and five with another diagnosis developed a significant disease relapse (n = 7) or adverse events (n = 5) within 2 years; 10 of these patients discontinued Remsima® treatment, one withdrew from the study and one received additional corticosteroid therapy. Conclusions: We observed no significant differences in PSROs, PPDA and laboratory parameters after treatment was switched from Rem

Published
2020
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19. Rapid Low-Cost Microarray-Based Genotyping for Genetic Screening in Primary Immunodeficiency

Author

Suratannon, N. (Narissara), van Wijck, R.T.A. (Rogier T. A.), Broer, L. (Linda), Xue, L. (Laixi), Meurs, J.B.J. (Joyce) van, Barendregt, B.H. (Barbara), Burg, M. (Mirjam) van der, Dik, W.A. (Willem), Chatchatee, P. (Pantipa), Langerak, A.W. (Anton), Swagemakers, S.M.A. (Sigrid), Goos, J.A.C. (Jacqueline), Mathijssen, I.M.J. (Irene M. J.), Dalm, V.A.S.H. (Virgil), Suphapeetiporn, K. (Kanya), Heezen, K. (Kim), Drabwell, J. (Jose), Uitterlinden, A.G. (André), Spek, P.J. (Peter) van der, van Hagen, P.M. (P. Martin), Suratannon, N. (Narissara), van Wijck, R.T.A. (Rogier T. A.), Broer, L. (Linda), Xue, L. (Laixi), Meurs, J.B.J. (Joyce) van, Barendregt, B.H. (Barbara), Burg, M. (Mirjam) van der, Dik, W.A. (Willem), Chatchatee, P. (Pantipa), Langerak, A.W. (Anton), Swagemakers, S.M.A. (Sigrid), Goos, J.A.C. (Jacqueline), Mathijssen, I.M.J. (Irene M. J.), Dalm, V.A.S.H. (Virgil), Suphapeetiporn, K. (Kanya), Heezen, K. (Kim), Drabwell, J. (Jose), Uitterlinden, A.G. (André), Spek, P.J. (Peter) van der, and van Hagen, P.M. (P. Martin)

Abstract

Background: Genetic tests for primary immunodeficiency disorders (PIDs) are expensive, time-consuming, and not easily accessible in developing countries. Therefore, we studied the feasibility of a customized single nucleotide variant (SNV) microarray that we developed to detect disease-causing variants and copy number variation (CNV) in patients with PIDs for only 40 Euros. Methods: Probes were custom-designed to genotype 9,415 variants of 277 PID-related genes, and were added to the genome-wide Illumina Global Screening Array (GSA). Data analysis of GSA was performed using Illumina GenomeStudio 2.0, Biodiscovery Nexus 10.0, and R-3.4.4 software. Validation of genotype calling was performed by comparing the GSA with whole-genome sequencing (WGS) data of 56 non-PID controls. DNA samples of 95 clinically diagnosed PID patients, of which 60 patients (63%) had a genetically established diagnosis (by Next-Generation Sequencing (NGS) PID panels or Sanger sequencing), we

Published
2020
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20. No Evidence for Circulating Retina Specific Autoreactive T-cells in Latent Tuberculosis-associated Uveitis and Sarcoid Uveitis

Author

Schrijver, B. (Benjamin), Hardjosantoso, H. (Hannah), Berge, J.C.E.M. (Josianne) ten, Schreurs, M.W.J. (Marco), Van Hagen, P.M. (P. Martin), Brooimans, R.A. (Rik), Rothová, A. (Aniki), Dik, W.A. (Willem), Schrijver, B. (Benjamin), Hardjosantoso, H. (Hannah), Berge, J.C.E.M. (Josianne) ten, Schreurs, M.W.J. (Marco), Van Hagen, P.M. (P. Martin), Brooimans, R.A. (Rik), Rothová, A. (Aniki), and Dik, W.A. (Willem)

Abstract

Purpose: To detect circulating retina-specific autoreactive CD4+ T-cells and antiretinal antibodies (ARA) in latent tuberculosis (TB)-associated uveitis or sarcoid uveitis patients. Methods: The presence of crude retinal extract (RE) autoreactive CD4+ T-cells was determined by a highly sensitive flowcytometric-based technique examining co-expression of CD25 and CD134 (OX40) on RE stimulated PBMC. The presence of ARA in available matched serum samples was assessed by indirect immunofluorescence. Results: No autoreactive CD4+ T-cells against RE could be detected in either latent TB-associated uveitis or sarcoid uveitis patients, while ARA were detected in the serum of the majority (5/6) of latent TB-associated uveitis and all (3/3) sarcoid uveitis patients. Conclusion: Even with the use of this highly sensitive flowcytometric technique circulating retina-specific autoreactive CD4+ T-cells could not be detected. In contrast, ARA were detected in the majority of patients indicating an adaptive humoral immune response toward retinal antigens had occurred.

Published
2020
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21. Extensive longitudinal immune profiling reveals sustained innate immune activaton in COVID-19 patients with unfavorable outcome

Author

IRAS OH Epidemiology Chemical Agents, dIRAS RA-2, Schrijver, B., Assmann, J.L.J.C., van Gammeren, A.J., Vermeulen, R.C.H., Portengen, L., Heukels, P., Langerak, A.W., Dik, W.A., van der Velden, V.H.J., Ermens, T.A.A.M., IRAS OH Epidemiology Chemical Agents, dIRAS RA-2, Schrijver, B., Assmann, J.L.J.C., van Gammeren, A.J., Vermeulen, R.C.H., Portengen, L., Heukels, P., Langerak, A.W., Dik, W.A., van der Velden, V.H.J., and Ermens, T.A.A.M.

Published
2020

22. Sensitivity and specificity of serum soluble interleukin-2 receptor for diagnosing sarcoidosis in a population of patients suspected of sarcoidosis

Author

Eurelings, L.E.M. (Laura E M), Miedema, J. (Jelle), Dalm, V.A.S.H. (Virgil), Daele, P.L.A. (Paul) van, van Hagen, P.M. (P Martin), Laar, J.A.M. (Jan) van, Dik, W.A. (Willem), Eurelings, L.E.M. (Laura E M), Miedema, J. (Jelle), Dalm, V.A.S.H. (Virgil), Daele, P.L.A. (Paul) van, van Hagen, P.M. (P Martin), Laar, J.A.M. (Jan) van, and Dik, W.A. (Willem)

Abstract

BACKGROUND: The soluble interleukin 2 receptor (sIL-2R) has been proposed as a marker of disease activity in patients with sarcoidosis. However, no studies have evaluated whether serum sIL-2R measurement is of use in establishing the diagnosis of sarcoidosis in patients who are suspected of sarcoidosis among other diseases. METHODS: A cohort study was conducted, consisting of new patients who visited the immunology outpatient clinic and whose serum sIL-2R levels were available before a definitive diagnosis was established between February 2011 and February 2016. All patients underwent standard diagnostic testing for sarcoidosis (e.g. laboratory tests, radiographic and/or nuclear imaging and/or affected site biopsy). This resulted either in the diagnosis of sarcoidosis or the exclusion of sarcoidosis with the diagnosis of another disease. Results of sIL-2R and angiotensin-converting enzyme (ACE) levels, radiographic and nuclear imaging and histology results were collected and definitive diagnoses were recorded. Sensitivity, specificity, the concordance statistic from the receiver operating characteristic curve and Youden's Index were calculated to assess the performance of sIL-2R in the diagnosis of sarcoidosis and were compared to ACE, currently one of the most used diagnostic biomarkers in the diagnosis of sarcoidosis. RESULTS: In total 983 patients were screened for inclusion, of which 189 patients met the inclusion criteria. A total of 101 patients were diagnosed with sarcoidosis after diagnostic workup, of whom 79 were biopsy-proven. In 88 patients a diagnosis other than sarcoidosis was made. The sensitivity and specificity of serum soluble interleukin 2 receptor levels to detect sarcoidosis were 88% and 85%. The sensitivity and specificity of ACE were 62% and 76%. Receiver operating characteristic curve analysis revealed that sIL-2R receptor is superior to ACE (p<0.0001). CONCLUSION: Serum sIL-2R is a sensitive biomarker and superior to ACE in establishing the

Published
2019
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23. Circulating proangiogenic cells and proteins in patients with glioma and acute myocardial infarction: Differences in neovascularization between neoplasia and tissue regeneration

Author

Huizer, K. (Karin), Sacchetti, A. (Andrea), Dik, W.A. (Willem), Mustafa, D.A.M. (Dana), Kros, J.M. (Johan), Huizer, K. (Karin), Sacchetti, A. (Andrea), Dik, W.A. (Willem), Mustafa, D.A.M. (Dana), and Kros, J.M. (Johan)

Abstract

Although extensive angiogenesis takes place in glial tumors, antiangiogenic therapies have remained without the expected success. In the peripheral circulation of glioma patients, increased numbers of endothelial precursor cells (EPCs) are present, potentially offering targets for antiangiogenic therapy. However, for an antiangiogenic therapy to be successful, the therapy should specifically target glioma-related EPC subsets and secreted factors only. Here, we compared the EPC subsets and plasma factors in the peripheral circulation of patients with gliomas to acute myocardial infarctions. We investigated the five most important EPC subsets and 21 angiogenesis-related plasma factors in peripheral blood samples of 29 patients with glioma, 14 patients with myocardial infarction, and 20 healthy people as controls, by FACS and Luminex assay. In GBM patients, all EPC subsets were elevated as compared to healthy subjects. In addition, HPC and KDR+ cell fractions were higher than in MI, while CD133+ and KDR+CD133+ cell fractions were lower. There were differences in relative EPC fractions between the groups: KDR+ cells were the largest fraction in GBM, while CD133+ cells were the largest fraction in MI. An increase in glioma malignancy grade coincided with an increase in the KDR+ fraction, while the CD133+ cell fraction decreased relatively. Most plasma angiogenic factors were higher in GBM than in MI patients. In both MI and GBM, the ratio of CD133+ HPCs correlated significantly with elevated levels of MMP9. In the GBM patients, MMP9 correlated strongly with levels of all HPCs. In conclusion, the data demonstrate that EPC traffic in patients with glioma, representing neoplasia, is different from that in myocardial infarction, representing tissue regeneration. Glioma patients may benefit from therapies aimed at lowering KDR+ cells and HPCs.

Published
2019
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24. Highlighting the Role of Biomarkers of Inflammation in the Diagnosis and Management of Complex Regional Pain Syndrome

Author

Bharwani, K.D. (Krisna), Dik, W.A. (Willem), Dirckx, M. (Maaike), Huygen, F.J.P.M. (Frank), Bharwani, K.D. (Krisna), Dik, W.A. (Willem), Dirckx, M. (Maaike), and Huygen, F.J.P.M. (Frank)

Abstract

Complex regional pain syndrome (CRPS) is characterized by continuous pain that is often accompanied by sensory, motor, vasomotor, sudomotor, and trophic disturbances. If left untreated, it can have a significant impact on the quality of life of patients. The diagnosis of CRPS is currently based on a set of relatively subjective clinical criteria: the New International Association for the Study of Pain clinical diagnostic criteria for CRPS. There are still no objective laboratory tests to diagnose CRPS and there is a great need for simple, objective, and easily measurable biomarkers in the diagnosis and management of this disease. In this review, we discuss the role of inflammation in the multi-mechanism pathophysiology of CRPS and highlight the application of potential biomarkers of inflammation in the diagnosis and management of this disease.

Published
2019
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25. Efficacy of Baricitinib in the Treatment of Chilblains Associated With Aicardi-Goutières Syndrome, a Type I Interferonopathy

Author

Meesilpavikkai, K. (Kornvalee), Dik, W.A. (Willem), Schrijver, B. (Benjamin), Helden-Meeuwsen, C.G. (Cornelia) van, Versnel, M.A. (Marjan), Hagen, P.M. (Martin) van, Bijlsma, E.K. (Emilia), Ruivenkamp, C.A. (Claudia), Oele, M.J. (Margreet J.), Dalm, V.A.S.H. (Virgil), Meesilpavikkai, K. (Kornvalee), Dik, W.A. (Willem), Schrijver, B. (Benjamin), Helden-Meeuwsen, C.G. (Cornelia) van, Versnel, M.A. (Marjan), Hagen, P.M. (Martin) van, Bijlsma, E.K. (Emilia), Ruivenkamp, C.A. (Claudia), Oele, M.J. (Margreet J.), and Dalm, V.A.S.H. (Virgil)

Published
2019
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26. Type 1 interferon-inducible gene expression in QuantiFERON Gold TB-positive uveitis: A tool to stratify a high versus low risk of active tuberculosis?

Author

La Distia Nora, R. (Rina), Sitompul, R. (Ratna), Bakker, M. (Marleen), Versnel, M.A. (Marjan), Swagemakers, S.M.A. (Sigrid), van der Spek, P.J. (Peter J.), Susiyanti, M. (Made), Edwar, L. (Lukman), Sjamsoe, S. (Soedarman), Singh, G. (Gurmeet), Handayani, R.D. (Rr Diah), Rothová, A. (Aniki), Hagen, P.M. (Martin) van, Dik, W.A. (Willem), La Distia Nora, R. (Rina), Sitompul, R. (Ratna), Bakker, M. (Marleen), Versnel, M.A. (Marjan), Swagemakers, S.M.A. (Sigrid), van der Spek, P.J. (Peter J.), Susiyanti, M. (Made), Edwar, L. (Lukman), Sjamsoe, S. (Soedarman), Singh, G. (Gurmeet), Handayani, R.D. (Rr Diah), Rothová, A. (Aniki), Hagen, P.M. (Martin) van, and Dik, W.A. (Willem)

Abstract

QuantiFERON-Gold TB (QFT)-positive patients with undetermined cause of uveitis are problematic in terms of whether to diagnose and treat them for tuberculosis (TB). Here, we investigated whether peripheral blood expression of type 1 interferon (IFN)-inducible genes may be of use to stratify QFT-positive patients with uveitis into groups of high versus low risk of having active TB-associated uveitis. We recruited all new uveitis patients in Cipto Mangunkusumo Hospital, Jakarta, Indonesia for one year. We included 12 patients with uveitis and clinically diagnosed active pulmonary TB, 58 QFT-positive patients with uveitis of unknown cause, 10 newly diagnosed sputum-positive active pulmonary TB patients without uveitis and 23 QFT-negative healthy controls. Expression of 35 type 1 IFN-inducible genes was measured in peripheral blood cells from active pulmonary TB patients without uveitis and healthy controls. Differentially expressed genes were identified and used for further clustering analyses of the uveitis groups. A type-1 IFN gene signature score was calculated and the optimal cut-off value for this score to differentiate active pulmonary TB from healthy controls was determined and applied to QFT-positive patients with uveitis of unknown cause. Ten type 1 IFN-inducible genes were differentially expressed between active pulmonary TB and healthy controls. Expression of these 10 genes in QFT-positive patients with uveitis of unknown cause revealed three groups: 1); patients resembling active pulmonary TB, 2); patients resembling healthy controls, and 3); patients displaying an in-between gene expression pattern. A type 1 IFN gene signature score ≥5.61 displayed high sensitivity (100%) and specificity (91%) for identification of active TB. Application of this score to QFT-positive patients with uveitis of unknown cause yielded two groups with expected different likelihood (high vs. low) of having active-TB uveitis, and therefore may be useful in clinical management deci

Published
2018
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27. Soluble interleukin-2 receptor: A potential marker for monitoring disease activity in IgG4-related disease

Author

Karim, A.F. (Faiz), Eurelings, L.E.M. (L. E.M.), Bansie, R. (Rakesh), Hagen, P.M. (Martin) van, Laar, J.A.M. (Jan) van, Dik, W.A. (Willem), Karim, A.F. (Faiz), Eurelings, L.E.M. (L. E.M.), Bansie, R. (Rakesh), Hagen, P.M. (Martin) van, Laar, J.A.M. (Jan) van, and Dik, W.A. (Willem)

Abstract

Background. IgG4-related disease (IgG4-RD) is a fibroinflammatory condition. T-cells play a crucial role in the pathogenesis, and therefore, serum soluble interleukin-2 receptor (sIL-2R) may be a potential biomarker. Method. We studied the levels of sIL-2R in 26 histologically proven IgG4-RD patients with available serum sIL-2R and compared them to those in newly diagnosed and untreated sarcoidosis patients (n = 78) and controls (n = 101) and the serum sIL-2R levels in patients after treatment of IgG4- RD (n = 15). The disease activity was measured using the IgG4-Related Disease Responder Index (IgG4-RD RI). Results. Median serum sIL-2R in IgG4-RD patients was 4667 pg/ml compared to 1515 pg/ml in controls (P < 0 001) and 6050 pg/ml in sarcoidosis patients (P = 0 004 compared to IgG4-RD). All IgG4-RD patients had elevated serum sIL-2R levels compared to the reference value of < 2500 pg/ml in controls and 85% elevated serum IgG4; however, these did not correlate with each other. Both serum sIL-2R and IgG4 levels declined significantly after treatment (P = 0 001 and P = 0 01, resp.). Before treatment, serum sIL- 2R level and IgG4-RD RI did not correlate with each other. However, the decrease in serum sIL-2R upon treatment did correlate significantly (P = 0 04) with the decrease in disease activity assessed by IgG-RD RI. Conclusion. Serum sIL-2R is elevated in IgG4-RD reflecting the inflammatory process with enhanced T-cell activation. Furthermore, serum sIL-2R might serve as a potential marker of response to treatment in IgG4-RD.

Published
2018
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28. Elevated Plasma Levels of sIL-2R in Complex Regional Pain Syndrome: A Pathogenic Role for T-Lymphocytes?

Author

Bharwani, K.D. (Krisna), Dirckx, M. (Maaike), Stronks, D.L. (Dirk), Dik, W.A. (Willem), Schreurs, M.W.J. (Marco), Huygen, F.J.P.M. (Frank), Bharwani, K.D. (Krisna), Dirckx, M. (Maaike), Stronks, D.L. (Dirk), Dik, W.A. (Willem), Schreurs, M.W.J. (Marco), and Huygen, F.J.P.M. (Frank)

Abstract

The immune system has long been thought to be involved in the pathophysiology of complex regional pain syndrome (CRPS). However, not much is known about the role of the immune system and specifically T-cells in the onset and maintenance of this disease. In this study, we aimed to evaluate T-cell activity in CRPS by comparing blood soluble interleukin-2 receptor (sIL-2R) levels between CRPS patients and healthy controls. CRPS patients had statistically significant elevated levels of sIL-2R as compared to healthy controls (median sIL-2R levels

Published
2017
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29. The identification of celiac disease in asymptomatic children: the Generation R Study

Author

Jansen, M.A.E. (Michelle), Zelm, M.C. (Menno) van, Groeneweg, M. (Michael), Jaddoe, V.W.V. (Vincent), Dik, W.A. (Willem), Schreurs, M.W.J. (Marco), Hooijkaas, H. (Herbert), Moll, H.A. (Henriëtte), Escher, J.C. (Johanna), Jansen, M.A.E. (Michelle), Zelm, M.C. (Menno) van, Groeneweg, M. (Michael), Jaddoe, V.W.V. (Vincent), Dik, W.A. (Willem), Schreurs, M.W.J. (Marco), Hooijkaas, H. (Herbert), Moll, H.A. (Henriëtte), and Escher, J.C. (Johanna)

Abstract

Background: The objective of our study was to assess whether TG2A levels in the healthy childhood population can be predictive of subclinical CD. Methods: A total of 4442 children (median age, 6.0 years) participating in a population-based prospective cohort study were screened on serum TG2A. Those with positive TG2A (≥7 U/ml; n = 60, 1.4%) were invited for clinical evaluation (median age, 9.0 years). Medical history, physical examination, serum TG2A, and IgA-endomysium (EMA) were assessed, as well as HLA DQ 2.2/2.5/8 typing. Patients with positive serologies and genetic risk types underwent duodenal biopsies. TG2A levels at the time of biopsy were compared with the degree of enteropathy. Results: Fifty-one TG2A-positive children were included in the follow-up: 31 (60.8%) children had CD, ten (19.6%) did not have CD, and ten (19.6%) were considered potential CD cases because of inconclusive serologies. Duodenal biopsies were performed in 26/31 children. CD with Marsh 3a/b enteropathy was observed in 75% (15/20) of children having TG2A levels ≥10ULN at 6 years of age, as well as in 75% (6/8) of children having a positive TG2A <10 ULN (OR 1.00; 95% CI 0.15–6.64). CD cases had a lower BMI SDS (mean −0.49, SD 0.92) than children without CD (mean 0.47, SD 1.37; p = 0.02). No differences were observed in gastrointestinal symptoms. Conclusions: Serum TG2A screening at 6 years of age in the healthy childhood population has a positive predictive value of 61% to detect subclinical CD. We did not find a positive correlation between serum TG2A levels and the degree of enteropathy.

Published
2017
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30. A novel heterozygous mutation in the STAT1 SH2 domain causes chronic mucocutaneous candidiasis, atypically diverse infections, autoimmunity, and impaired cytokine regulation

Author

Meesilpavikkai, K. (Kornvalee), Dik, W.A. (Willem), Schrijver, B. (Benjamin), Nagtzaam, N.M. (Nicole), Rijswijk, A.L. (Angelique), Driessen, G.J.A. (Gertjan), Spek, P.J. (Peter) van der, Hagen, P.M. (Martin) van, Dalm, V.A.S.H. (Virgil), Meesilpavikkai, K. (Kornvalee), Dik, W.A. (Willem), Schrijver, B. (Benjamin), Nagtzaam, N.M. (Nicole), Rijswijk, A.L. (Angelique), Driessen, G.J.A. (Gertjan), Spek, P.J. (Peter) van der, Hagen, P.M. (Martin) van, and Dalm, V.A.S.H. (Virgil)

Abstract

Chronic mucocutaneous candidiasis (CMC) is a primary immunodeficiency characterized by persistent or recurrent skin and mucosal surface infections with Candida species. Different gene mutations leading to CMC have been identified. These include various heterozygous gain-of-function (GOF) mutations in signal transducer and activator of transcription 1 (STAT1) that are not only associated with infections but also with autoimmune manifestations. Recently, two STAT1 GOF mutations involving the Src homology 2 (SH2) domain have been reported, while so far, over 50 mutations have been described mainly in the coiled coil and the DNA-binding domains. Here, we present two members of a Dutch family with a novel STAT1 mutation located in the SH2 domain. T lymphocytes of these patients revealed STAT1 hyperphosphorylation and higher expression of STAT1 target genes. The clinical picture of CMC in our patients could be explained by diminished production of interleukin (IL)-17 and IL-22, cytokines important in the protection against fungal infections.

Published
2017
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31. The interferon type I signature is present in systemic sclerosis before overt fibrosis and might contribute to its pathogenesis through high BAFF gene expression and high collagen synthesis

Author

Brkic, Z., Bon, L. van, Cossu, M., Helden-Meeuwsen, C.G. van, Vonk, M.C., Knaapen, H., Berg, W. van den, Dalm, V.A., Daele, P.L. van, Severino, A., Maria, N.I., Guillen, S., Dik, W.A., Beretta, L., Versnel, M.A., Radstake, T., Brkic, Z., Bon, L. van, Cossu, M., Helden-Meeuwsen, C.G. van, Vonk, M.C., Knaapen, H., Berg, W. van den, Dalm, V.A., Daele, P.L. van, Severino, A., Maria, N.I., Guillen, S., Dik, W.A., Beretta, L., Versnel, M.A., and Radstake, T.

Abstract

Contains fulltext : 171751.pdf (publisher's version ) (Closed access), BACKGROUND: Interferon (IFN) signature has been reported in definite systemic sclerosis (SSc) but it has not been characterised in early SSc (EaSSc). We aim at characterising IFN type I signature in SSc before overt skin fibrosis develops. METHODS: The expression of 11 IFN type I inducible genes was tested in whole-blood samples from 30 healthy controls (HCs), 12 subjects with primary Raynaud's phenomenon (RP), 19 patients with EaSSc, 7 patients with definite SSc without cutaneous fibrosis, 21 limited cutaneous SSc and 10 diffuse cutaneous SSc subjects. The correlation between IFN activity in monocytes, B cell activating factor (BAFF) mRNA expression and type III procollagen N-terminal propeptide (PIIINP) serum levels was tested. RESULTS: In all the SSc groups, higher IFN scores were observed compared with HC. An IFN score >/=7.09 discriminated HCs from patients with SSc (sensitivity=0.7, specificity=0.88, area under receiving operating characteristic (AUROC)=0.82); the prevalence of an elevated IFN score was: HC=3.3%; RP=33.3%, EaSSc=78.9%, definite SSc=100%, limited cutaneous SSc=42.9%, diffuse cutaneous SSc=70.0%. In monocytes an IFN score >/=4.12 distinguished HCs from patients with fibrotic SSc (sensitivity=0.62, specificity=0.85, AUROC=0.76). Compared with IFN-negative subjects, IFN-positive subjects had higher monocyte BAFF mRNA levels (19.7+/-5.2 vs 15.20+/-4.0, p=2.1x10(-5)) and serum PIIINP levels (median=6.0 (IQR 5.4-8.9) vs median=3.9 (IQR 3.3-4.7), p=0.0004). CONCLUSIONS: An IFN type I signature is observed in patients with SSc from the earliest phases of the disease, even before overt skin fibrosis. The presence of IFN type I signature in monocytes is correlated with BAFF mRNA expression and serum PIIINP levels, supporting a contribution in the pathogenesis and progression of SSc.

Published
2016

32. Basic FGF and PDGF-BB synergistically stimulate hyaluronan and IL-6 production by orbital fibroblasts

Author

Virakul, S. (Sita), Heutz, J.W. (Judith W.), Dalm, V.A.S.H. (Virgil), Peeters, R.P. (Robin), Paridaens, A.D.A. (Dion), Bosch, W.A. (Willem) van den, Hirankarn, N. (Nattiya), Hagen, P.M. (Martin) van, Dik, W.A. (Willem), Virakul, S. (Sita), Heutz, J.W. (Judith W.), Dalm, V.A.S.H. (Virgil), Peeters, R.P. (Robin), Paridaens, A.D.A. (Dion), Bosch, W.A. (Willem) van den, Hirankarn, N. (Nattiya), Hagen, P.M. (Martin) van, and Dik, W.A. (Willem)

Abstract

Orbital fibroblast activation is a central pathologic feature of Graves' Ophthalmopathy (GO). Basic fibroblast growth factor (bFGF) and vascular endothelial growth factor (VEGF) have been proposed to contribute to GO, but their effects on orbital fibroblasts are largely unknown.We found that bFGF stimulated proliferation and hyaluronan production, but not IL-6 production by orbital fibroblasts, while VEGF hardly affected orbital fibroblast activity. Remarkably, co-stimulation of orbital fibroblasts with bFGF and PDGF-BB synergistically enhanced IL-6 and hyaluronan production and displayed an additive effect on proliferation compared to either bFGF or PDGF-BB stimulation. Nintedanib, a FGF- and PDGF-receptor targeting drug, more efficiently blocked bFGF + PDGF-BB-induced IL-6 and hyaluronan production than dasatinib that only targets PDGF-receptor.In conclusion, bFGF may contribute to orbital inflammation and tissue remodeling in GO, especially through synergistic interaction with PDGF-BB. Multi-target therapy directed at the bFGF and PDGF pathways may potentially be of interest for the treatment of GO.

Published
2016
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34. Interferon-gamma immunotherapy in a patient with refractory disseminated candidiasis

Author

Buddingh, E.P., Leentjens, J., Lugt, J. van der, Dik, W.A., Gresnigt, M.S., Netea, M.G., Pickkers, P., Driessen, G.J., Buddingh, E.P., Leentjens, J., Lugt, J. van der, Dik, W.A., Gresnigt, M.S., Netea, M.G., Pickkers, P., and Driessen, G.J.

Abstract

Contains fulltext : 152382.pdf (publisher's version ) (Closed access), Despite advances in supportive care and novel antifungal agents, mortality due to invasive Candida infection is high. Athree-year-old boy with disseminatedC.dubliniensis infection during induction chemotherapy for acute lymphoblastic leukemiadeteriorated despite resolution of neutropenia and appropriate antifungal treatment. Monocyte HLA-DR-expression was extremely low, suggesting immunoparalysis. Adjuvant immunotherapy with IFN-gamma restored the immune response, which was accompanied by clinical and radiographic recovery.

Published
2015

36. The peripheral blood compartment in patients with Graves' disease: Activated T lymphocytes and increased transitional and pre-naive mature B lymphocytes

Author

Weerd, K. (Kim) van der, Hagen, P.M. (Martin) van, Schrijver, B. (Benjamin), Kwekkeboom, D.J. (Dirk Jan), Herder, W.W. (Wouter) de, Broek, M.R.J. ten, Postema, P.T.E. (Pieter), Dongen, J.J.M. (Jacques) van, Staal, F.J.T. (Frank), Dik, W.A. (Willem), Weerd, K. (Kim) van der, Hagen, P.M. (Martin) van, Schrijver, B. (Benjamin), Kwekkeboom, D.J. (Dirk Jan), Herder, W.W. (Wouter) de, Broek, M.R.J. ten, Postema, P.T.E. (Pieter), Dongen, J.J.M. (Jacques) van, Staal, F.J.T. (Frank), and Dik, W.A. (Willem)

Abstract

Graves' disease (GD) is an autoimmune disease that involves aberrant B and T lymphocyte responses. Detailed knowledge about lymphocyte subpopulation composition will therefore enhance our understanding of the pathogenesis of GD and might support the development of new immunomodulatory treatment approaches. The aim of this study was to gain detailed insight into the composition of the peripheral blood lymphocyte compartment in GD before and during anti-thyroid drug therapy. Major B and T lymphocyte subpopulations were investigated by flow cytometry in peripheral blood from newly diagnosed GD patients (n=5), GD patients treated with

Published
2013
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37. Breakpoint sites disclose the role of the V(D)J recombination machinery in the formation of T-cell receptor (TCR) and non-TCR associated aberrations in T-cell acute lymphoblastic leukemia

Author

Larmonie, N.S.D. (Nicole), Dik, W.A. (Willem), Meijerink, J.P.P. (Jules), Homminga, I. (Irene), Dongen, J.J.M. (Jacques) van, Langerak, A.W. (Anton), Larmonie, N.S.D. (Nicole), Dik, W.A. (Willem), Meijerink, J.P.P. (Jules), Homminga, I. (Irene), Dongen, J.J.M. (Jacques) van, and Langerak, A.W. (Anton)

Abstract

Aberrant recombination between T-cell receptor genes and oncogenes gives rise to chromosomal translocations that are genetic hallmarks in several subsets of human T-cell acute lymphoblastic leukemias. The V(D)J recombination machinery has been shown to play a role in the formation of these T-cell receptor translocations. Other, non-T-cell receptor chromosomal aberrations, such as SIL-TAL1 deletions, have likewise been recognized as V(D)J recombination associated aberrations. Despite the postulated role of V(D)J recombination, the extent of the V(D)J recombination machinery involvement in the formation of T-cell receptor and non-T-cell receptor aberrations in T-cell acute lymphoblastic leukem

Published
2013
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38. Morbidly obese human subjects have increased peripheral blood CD4 + T cells with skewing toward a Treg- and Th2-dominated phenotype

Author

Weerd, K. (Kim) van der, Dik, W.A. (Willem), Schrijver, B. (Benjamin), Schweitzer, D.H. (Dave ), Langerak, A.W. (Anton), Drexhage, H.A. (Hemmo), Kiewiet-Kemper, R.M. (Rosalie), Aken, M.O. (Maarten) van, Huisstede, A. (Astrid) van, Dongen, J.J.M. (Jacques) van, Lelij, A.J. (Aart Jan) van der, Staal, F.J.T. (Frank), Hagen, P.M. (Martin) van, Weerd, K. (Kim) van der, Dik, W.A. (Willem), Schrijver, B. (Benjamin), Schweitzer, D.H. (Dave ), Langerak, A.W. (Anton), Drexhage, H.A. (Hemmo), Kiewiet-Kemper, R.M. (Rosalie), Aken, M.O. (Maarten) van, Huisstede, A. (Astrid) van, Dongen, J.J.M. (Jacques) van, Lelij, A.J. (Aart Jan) van der, Staal, F.J.T. (Frank), and Hagen, P.M. (Martin) van

Abstract

Obesity is associated with local T-cell abnormalities in adipose tissue. Systemic obesity-related abnormalities in the peripheral blood T-cell compartment are not well defined. In this study, we investigated the peripheral blood T-cell compartment of morbidly obese and lean subjects. We determined all major T-cell sub-populations via six-color flow cytometry, including CD8+and CD4+T cells, CD4+T-helper (Th) subpopulations, and natural CD4+CD25+FoxP3+

Published
2012
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39. PDGF enhances orbital fibroblast responses to TSHR stimulating autoantibodies in Graves' ophthalmopathy patients

Author

Steensel, L. (Leendert) van, Hooijkaas, H. (Herbert), Paridaens, A.D.A. (Dion), Bosch, W.A. (Willem) van den, Kuijpers, R.W.A.M. (Robert), Drexhage, H.A. (Hemmo), Hagen, P.M. (Martin) van, Dik, W.A. (Willem), Steensel, L. (Leendert) van, Hooijkaas, H. (Herbert), Paridaens, A.D.A. (Dion), Bosch, W.A. (Willem) van den, Kuijpers, R.W.A.M. (Robert), Drexhage, H.A. (Hemmo), Hagen, P.M. (Martin) van, and Dik, W.A. (Willem)

Abstract

Purpose: Thyroid-stimulating hormone receptor (TSHR) stimulating autoantibodies are associated with Graves' ophthalmopathy (GO), the orbital manifestation of Graves' disease (GD). TSHR autoantibody levels and orbital TSHR expression levels correlate positively with GO disease activity. Platelet-derived growth factors (PDGF) are increased in GO and potently activate orbital fibroblast effector functions. We investigated the possible relationship between PDGF and TSHR expression on orbital fibroblasts and how that influences the immunopathological effects of TSHR autoantibodies on orbital fibroblast activity. Methods: Orbital fibroblasts were stimulated with PDGF-AA, PDGF-AB, and PDGF-BB, and TSHR expression was determined by flow cytometry. Stimulatory effects of bovine TSH and GD immunoglobulins on orbital fibroblasts (with or without PDGF-BB preincubation) were determined by IL-6, IL-8, chemokine (C-C motif) ligand (CCL)-2, CCL5, CCL7, and hyaluronan ELISA. The TSHR blocking antibody K1-70 and the cAMP inhibitor H89 were used to determine involvement of TSHR signaling. Results: PDGF-AB and PDGF-BB stimulation increased TSHR expression on orbital fibroblasts, whereas PDGF-AA did not. Furthermore, stimulation with bovine TSH and immunoglobulins from GD patients induced IL-6, IL-8, CCL2, and hyaluronan production by orbital fibroblasts, and PDGF-BB preincubation enhanced this response of orbital fibroblasts. Blocking studies with a TSHR blocking antibody and a cAMP inhibitor inhibited these effects, indicating the involvement of TSHR signaling and thus of TSHR stimulating autoantibodies herein. Conclusions: These findings indicate that PDGF-B containing PDGF isoforms amplify the immunopathological effects of TSHR-stimulating autoantibodies in GO patients by stimulating TSHR expression on orbital fibroblasts. Copyright

Published
2012
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40. Posttranscriptional deregulation of MYC via PTEN constitutes a major alternative pathway of MYC activation in T-cell acute lymphoblastic leukemia

Author

Bonnet, M. (Mélanie), Loosveld, M. (Marie), Montpellier, B. (Bertrand), Navarro, J.-M., Quilichini, B. (Benoit), Picard, C. (Christophe), Cristofaro, J.D., Bagnis, C. (Claude), Fossat, C. (Chantal), Hernandez, L. (Lucie), Mamessier, E. (Emilie), Roulland, S. (Sandrine), Morgado, E. (Ester), Formisano-Tréziny, C. (Christine), Dik, W.A. (Willem), Langerak, A.W. (Anton), Prebet, T. (Thomas), Vey, N. (Norbert), Michel, G. (Gérard), Gabert, J. (Jean), Soulier, J. (Jean), Macintyre, E., Asnafi, V. (Vahid), Payet-Bornet, D. (Dominique), Nadel, B. (Bertrand), Bonnet, M. (Mélanie), Loosveld, M. (Marie), Montpellier, B. (Bertrand), Navarro, J.-M., Quilichini, B. (Benoit), Picard, C. (Christophe), Cristofaro, J.D., Bagnis, C. (Claude), Fossat, C. (Chantal), Hernandez, L. (Lucie), Mamessier, E. (Emilie), Roulland, S. (Sandrine), Morgado, E. (Ester), Formisano-Tréziny, C. (Christine), Dik, W.A. (Willem), Langerak, A.W. (Anton), Prebet, T. (Thomas), Vey, N. (Norbert), Michel, G. (Gérard), Gabert, J. (Jean), Soulier, J. (Jean), Macintyre, E., Asnafi, V. (Vahid), Payet-Bornet, D. (Dominique), and Nadel, B. (Bertrand)

Abstract

Cumulative evidence indicates that MYC, one of the major downstream effectors of NOTCH1, is a critical component of T-cell acute lymphoblastic leukemia (T-ALL) oncogenesis and a potential candidate for targeted therapy. However, MYC is a complex oncogene, involving both fine protein dosage and cell-context dependency, and detailed understanding of MYC-mediated oncogenesis in T-ALL is still lacking. To better understand how MYC is interspersed in the complex T-ALL oncogenic networks, we performed a thorough molecular and biochemical analysis of MYC activation in a comprehensive collection of primary adult and pediatric patient samples. We find that MYC expression is highly variable, and that high MYC expression levels can be generated in a large number of cases in absence of NOTCH1/FBXW7 mutations, suggesting the occurrence of multiple activation pathways in addition to NOTCH1. Furthermore, we show that posttranscriptional deregulation of MYC constitutes a major alternative pathway of MYC activation in T-ALL, operating partly via the PI3K/AKT axis through down-regulation of PTEN, and that NOTCH1mmight play a dual transcriptional and posttranscriptional role in this process. Altogether, our data lend further support to the significance of therapeutic targeting of MYC and/or the PTEN/AKT pathways, both in GSI-resistant and identified NOTCH1-independent/MYC-mediated T-ALL patients.

Published
2011
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41. Mitigation of septic shock in mice and rhesus monkeys by human chorionic gonadotrophin-related oligopeptides

Author

Khan, N.A. (Nisar Ahmed), Vierboom, M.P.M. (Michel), Holten-Neelen, C. (Conny) van, Breedveld, E. (Elly), Zuiderwijk-Sick, E.A. (Ella), Khan, A., Kondova, I. (Ivanela), Braskamp, G., Savelkoul, H.F.J. (Huub), Dik, W.A. (Willem), Thart, B.A., Benner, R. (Robbert), Khan, N.A. (Nisar Ahmed), Vierboom, M.P.M. (Michel), Holten-Neelen, C. (Conny) van, Breedveld, E. (Elly), Zuiderwijk-Sick, E.A. (Ella), Khan, A., Kondova, I. (Ivanela), Braskamp, G., Savelkoul, H.F.J. (Huub), Dik, W.A. (Willem), Thart, B.A., and Benner, R. (Robbert)

Abstract

The marked improvement of several immune-mediated inflammatory diseases during pregnancy has drawn attention to pregnancy hormones as potential therapeutics for such disorders. Low molecular weight fractions derived from the pregnancy hormone human chorionic gonadotrophin (hCG) have remarkable potent immunosuppressive effects in mouse models of diabetes and septic shock. Based on these data we have designed a set of oligopeptides related to the primary structure of hCG and tested these in models of septic shock in mice and rhesus monkeys. We demonstrate that mice exposed to lipopolysaccharide (LPS) and treated subsequently with selected tri-, tetra-, penta- and hepta-meric oligopeptides (i.e. MTR, VVC, MTRV, LQGV, AQGV, VLPALP, VLPALPQ) are protected against fatal LPS-induced septic shock. Moreover, administration of a cocktail of three selected oligopeptides (LQGV, AQGV and VLPALP) improved the pathological features markedly and nearly improved haemodynamic parameters associated with intravenous Escherichia coli-induced septic shock in rhesus monkeys. These data indicate that the designed hCG-related oligopeptides may present a potential treatment for the initial hyperdynamic phase of septic shock in humans.

Published
2010
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42. Cytokines in the colon of a patient with Behçet's disease

Author

Kappen, J.H. (Jasper), Dik, W.A. (Willem), Dingjan, G.M. (Gemma), Daele, P.L.A. (Paul) van, Hooijkaas, H. (Herbert), Martin, M.P. (Martin), Laar, J.A.M. (Jan) van, Kappen, J.H. (Jasper), Dik, W.A. (Willem), Dingjan, G.M. (Gemma), Daele, P.L.A. (Paul) van, Hooijkaas, H. (Herbert), Martin, M.P. (Martin), and Laar, J.A.M. (Jan) van

Published
2009
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43. Human T-cell lines with well-defined T-cell receptor gene rearrangements as controls for the BIOMED-2 multiplex polymerase chain reaction tubes.

Author

Sandberg, Y., Verhaaf, B., Gastel-Mol, E.J. van, Wolvers-Tettero, I.L.M., Vos, J., Macleod, R.A., Noordzij, J.G., Dik, W.A., Dongen, J.J.M. van, Langerak, A.W., Sandberg, Y., Verhaaf, B., Gastel-Mol, E.J. van, Wolvers-Tettero, I.L.M., Vos, J., Macleod, R.A., Noordzij, J.G., Dik, W.A., Dongen, J.J.M. van, and Langerak, A.W.

Abstract

Item does not contain fulltext, The BIOMED-2 multiplex polymerase chain reaction (PCR) tubes for analysis of immunoglobulin and T-cell receptor (TCR) gene rearrangements have recently been introduced as a reliable and easy tool for clonality diagnostics in suspected lymphoproliferations. Quality and performance assessment of PCR-based clonality diagnostics is generally performed using human leukemia/lymphoma cell lines as controls. We evaluated the utility of 30 well-defined human T-cell lines for quality performance testing of the BIOMED-2 PCR primers and protocols. The PCR analyses of the TCR loci were backed up by Southern blot analysis. The clonal TCRB, TCRG and TCRD gene rearrangements were analyzed for gene segment usage and for the size and composition of their junctional regions. In 29 out of 30 cell lines, unique clonal TCR gene rearrangements could be easily detected. Besides their usefulness in molecular clonality diagnostics, these cell lines can now be authenticated based on their TCR gene rearrangement profile. This enables their correct use in molecular clonality diagnostics and in other cancer research studies.

Published
2007

44. New insights on human T cell development by quantitative T cell receptor gene rearrangement studies and gene expression profiling

Author

Dik, W.A. (Willem), Dongen, J.J.M. (Jacques) van, Staal, F.J.T. (Frank), Langerak, A.W. (Anton), Weerkamp, F. (Floor), Ridder, D. (Dick) de, Haas, E.F. (Edwin) de, Baert, M.R.M. (Miranda), Koster, E.E. (Esther), Reinders, M.J. (Marcel), Spek, P.J. (Peter) van der, Pike, K. (Karin), Dik, W.A. (Willem), Dongen, J.J.M. (Jacques) van, Staal, F.J.T. (Frank), Langerak, A.W. (Anton), Weerkamp, F. (Floor), Ridder, D. (Dick) de, Haas, E.F. (Edwin) de, Baert, M.R.M. (Miranda), Koster, E.E. (Esther), Reinders, M.J. (Marcel), Spek, P.J. (Peter) van der, and Pike, K. (Karin)

Abstract

To gain more insight into initiation and regulation of T cell receptor (TCR) gene rearrangement during human T cell development, we analyzed TCR gene rearrangements by quantitative PCR analysis in nine consecutive T cell developmental stages, including CD34+ lin- cord blood cells as a reference. The same stages were used for gene expression profiling using DNA microarrays. We show that TCR loci rearrange in a highly ordered way (TCRD-TCRG-TCRB-TCRA) and that the initiating Ddelta2-Ddelta3 rearrangement occurs at the most immature CD34+CD38-CD1a- stage. TCRB rearrangement starts at the CD34+CD38+CD1a- stage and complete in-frame TCRB rearrangements were first detected in the immature single positive stage. TCRB rearrangement data together with the PTCRA (pTalpha) expression pattern show that human TCRbeta-selection occurs at the CD34+CD38+CD1a+ stage. By combining the TCR rearrangement data with gene expression data, we identified candidate factors for the initiation/regulation of TCR recombination. Our data demonstrate that a number of key events occur earlier than assumed previously; therefore, human T cell development is much more similar to murine T cell development than reported before.

Published
2005

47. Dexamethasone treatment does not inhibit fibroproliferation in chronic lung disease of prematurity

Author

Dik, W.A. (Willem), Versnel, M.A. (Marjan), Naber, B.A. (Brigitta), Janssen, D.J.M.T. (Daphne), Kaam, A.H. van, Zimmermann, L.J.I. (Luc), Dik, W.A. (Willem), Versnel, M.A. (Marjan), Naber, B.A. (Brigitta), Janssen, D.J.M.T. (Daphne), Kaam, A.H. van, and Zimmermann, L.J.I. (Luc)

Abstract

Pulmonary fibrosis results from excessive fibroblast proliferation and increased collagen deposition and occurs in chronic lung disease of prematurity (CLD). Platelet-derived growth factor (PDGF)-BB is mitogenic for fibroblasts and levels are increased in fibrotic lung disorders. Systemic dexamethasone (DEX) treatment improves pulmonary function and reduces inflammation in infants with or at risk of CLD. However, the effect of DEX treatment on fibroblast activity, PDGF-BB and collagen synthesis in the lungs of CLD patients is uncertain. Bronchoalveolar lavage (BAL) fluids, obtained from 15 infants at risk of CLD before and after DEX treatment, were analysed for fibroblast mitogenicity, PDGF-BB, N-terminal propeptide of collagen type III (PIIINP) and interleukin

Published
2003

48. Short course dexamethasone treatment following injury inhibits bleomycin induced fibrosis in rats

Author

Dik, W.A. (Willem), McAnulty, R.J., Versnel, M.A. (Marjan), Naber, B.A. (Brigitta), Zimmermann, L.J.I. (Luc), Laurent, G.J., Mutsaers, S.E. (Steven), Dik, W.A. (Willem), McAnulty, R.J., Versnel, M.A. (Marjan), Naber, B.A. (Brigitta), Zimmermann, L.J.I. (Luc), Laurent, G.J., and Mutsaers, S.E. (Steven)

Abstract

BACKGROUND: Corticosteroids are routinely used in patients with pulmonary fibrosis. The timing for initiation of treatment is likely to be crucial for corticosteroids to exert an antifibrotic effect. Experimental studies in animals have examined the effect of corticosteroid treatment start

Published
2003
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50. Lung disease of the preterm infant: mediators involved in fibroproliferation and fibrogenesis

Author

Dik, W.A. (Willem) and Dik, W.A. (Willem)

Abstract

To save life. prematurely born infants with neonatal respiratory distress syndrome (RDS) are artificially ventilated. RDS can resolve within days after birth (uncomplicated RDS) or progress towards a chronic lung disease called bronchopulmonary dysplasia (BPD). The lung pathology of BPD is associated with varying degrees of fibrosis that develops within days to weeks after mechanical ventilation treatment for RDS. The development of pulmonary fibrosis generally follows an inflammatory phase and is characterized by an increase in pulmonary fibroblast numbers and increased deposition of extracellular matrix components (especially collagen) in the lung interstitium. Numerous studies have focussed on inflammatory mediators in the pathogenesis of BPD. but only a few reports are available on the presence of fibrogenic mediators in the lungs during BPD development. The studies described in this thesis focussed mainly on mediators known to be involved in fibroproliferation (fibroblast proliferation) and fibrogenesis (collagen deposition) and are. therefore, of interest in understanding the pathogenesis of BPD. When sequential BAL fluids were examined from infants with resolving RDS and from infants developing BPD for their ntitogenic activity for human fetal lung fibroblasts (HFL-1) no differences were observed. This suggests that the mitogenic activity in the lungs of prematurely born infants is associated with RDS resolution and contributes to (or reflects) repair of the injured lung structures. The infants that developed BPD. experienced more severe RDS than the resolving infants. This suggests that the infants with BPD development had more severe lung tissue damage than infants with resolving RDS. At postnatal days 2 to 7. the ntitogenic activity of BAL fluids was comparable between RDS and BPD. in contrast to the expectation that the BAL fl

Published
2002

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