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101. Evidence for enhanced Bruton's tyrosine kinase activity in transitional and naïve B cells of patients with granulomatosis with polyangiitis.

Author

Borstel, Anouk von, Abdulahad, Wayel H, Sanders, Jan Stephan, Rip, Jasper, Neys, Stefan F H, Hendriks, Rudi W, Stegeman, Coen A, Heeringa, Peter, Rutgers, Abraham, and Corneth, Odilia B J

Subjects
*B cells, *CELL receptors, *CYTOKINES, *FLOW cytometry, *IMMUNOGLOBULINS, *PHOSPHORYLATION, *PROTEIN-tyrosine kinases, *VASCULITIS, *GRANULOMATOSIS with polyangiitis, *CASE-control method, *ANTIBODY formation, *ANTINEUTROPHIL cytoplasmic antibodies, *CHEMICAL inhibitors
Abstract

Objectives To determine Bruton's tyrosine kinase (BTK) protein and phosphorylation levels in B cell subsets of granulomatosis with polyangiitis (GPA) patients and to investigate the effect of BTK blockade on in vitro B cell cytokine production, subset distribution and (auto)antibody production. Methods BTK protein and phosphorylation levels were determined by flow cytometry in peripheral blood B cells of 29 untreated GPA patients [9 active and 20 remission GPA patients (10 ANCA– and 10 ANCA+)], 9 age- and sex-matched healthy controls (HCs) and 9 untreated active RA patients. The effect of BTK blockade on in vitro B cell cytokine production, subset distribution and (auto)antibody production was determined in the same donors in peripheral blood mononuclear cell cultures. Results BTK protein levels were significantly increased in transitional and naïve B cells of active GPA and RA patients compared with remission GPA patients and HCs. Both B cell subsets of active patients were more sensitive to B cell receptor stimulation, as BTK and phospholipase Cγ2 phosphorylation were increased in these patients. In vitro BTK blockade had profound effects on B cell cytokine production, plasma cell formation and (auto)antibody production in both GPA patients and HCs. Interestingly, the effect of BTK blockade was less pronounced in active GPA patients, possibly due to increased activation of B cells. Conclusion We show that BTK protein and phosphorylation levels are most profoundly increased in newly emerging B cells of active GPA patients compared with remission patients. BTK blockade greatly inhibits in vitro B cell effector functions in GPA patients and HCs. These promising data identify BTK as an interesting novel therapeutic target in the treatment of GPA. [ABSTRACT FROM AUTHOR]

Published
2019
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102. CD27+CD38hi B Cell Frequency During Remission Predicts Relapsing Disease in Granulomatosis With Polyangiitis Patients.

Author

von Borstel, Anouk, Land, Judith, Abdulahad, Wayel H., Rutgers, Abraham, Stegeman, Coen A., Diepstra, Arjan, Heeringa, Peter, and Sanders, Jan Stephan

Subjects
B cells, GRANULOMATOSIS with polyangiitis, DISEASE relapse, CELL migration, CELLULAR inclusions
Abstract

Background: Granulomatosis with polyangiitis (GPA) patients are prone to disease relapses. We aimed to determine whether GPA patients at risk for relapse can be identified by differences in B cell subset frequencies. Methods: Eighty-five GPA patients were monitored for a median period of 3.1 years (range: 0.1–6.3). Circulating B cell subset frequencies were analyzed by flow cytometry determining the expression of CD19, CD38, and CD27. B cell subset frequencies at the time of inclusion of future-relapsing (F-R) and non-relapsing (N-R) patients were compared and related to relapse-free survival. Additionally, CD27+CD38hi B cells were assessed in urine and kidney biopsies from active anti-neutrophil cytoplasmic autoantibody-associated vasculitides (AAV) patients with renal involvement. Results: Within 1.6 years, 30% of patients experienced a relapse. The CD27+CD38hi B cell frequency at the time of inclusion was increased in F-R (median: 2.39%) compared to N-R patients (median: 1.03%; p = 0.0025) and a trend was found compared with the HCs (median: 1.33%; p = 0.08). This increased CD27+CD38hi B cell frequency at inclusion was correlated to decreased relapse-free survival in GPA patients. In addition, 74.7% of patients with an increased CD27+CD38hi B cell frequency (≥2.39%) relapsed during follow-up compared to 19.7% of patients with a CD27+CD38hi B cell frequency of <2.39%. No correlations were found between CD27+CD38hi B cells and ANCA levels. CD27+CD38hi B cell frequencies were increased in urine compared to the circulation, and were also detected in kidney biopsies, which may indicate CD27+CD38hi B cell migration during active disease. Conclusions: Our data suggests that having an increased frequency of circulating CD27+CD38hi B cells during remission is related to a higher relapse risk in GPA patients, and therefore might be a potential marker to identify those GPA patients at risk for relapse. [ABSTRACT FROM AUTHOR]

Published
2019
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103. Markers of angiogenesis and macrophage products for predicting disease course and monitoring vascular inflammation in giant cell arteritis.

Author

Sleen, Yannick van, Sandovici, Maria, Abdulahad, Wayel H, Bijzet, Johan, Geest, Kornelis S M van der, Boots, Annemieke M H, and Brouwer, Elisabeth

Subjects
THERAPEUTIC use of glucocorticoids, GIANT cell arteritis diagnosis, AMYLOID, BIOMARKERS, BIOLOGICAL assay, CALCIUM-binding proteins, CELL receptors, ENZYME-linked immunosorbent assay, GIANT cell arteritis, GLYCOPROTEINS, INTERLEUKINS, LONGITUDINAL method, MACROPHAGES, NEOVASCULARIZATION, DISEASE relapse, VASCULAR endothelial growth factors, TREATMENT effectiveness, DISEASE remission, BLOOD
Abstract

Objective GCA, a systemic vasculitis, is characterized by an IL-6-dependent acute-phase response. This response is typically suppressed by treatment rendering CRP/ESR unreliable for monitoring vascular inflammation. Also, there are no accurate biomarkers predicting a non-favourable disease course. Here we investigated macrophage products and markers of angiogenesis as biomarkers for prognosis and monitoring of vascular inflammation. Methods Forty-one newly diagnosed, glucocorticoid-naive GCA patients were prospectively followed for relapses and glucocorticoid requirement for a median of 30 months (range 0–71). Serum markers at baseline and during follow-up were compared with 33 age-matched healthy controls and 13 infection controls. Concentrations of IL-6, serum amyloid A, soluble CD163, calprotectin, YKL-40, VEGF, angiopoietin-1 and -2 and sTie2 were determined by ELISA/Luminex assay. Results Serum concentrations of all markers, but not angiopoietin-1, were elevated in GCA patients at baseline when compared with healthy controls. High VEGF (P = 0.0025) and angiopoietin-1 (P = 0.0174) and low YKL-40 (P = 0.0369) levels at baseline were predictive of a short time to glucocorticoid-free remission. Elevated angiopoietin-2 levels were associated with an imminent relapse during treatment (P < 0.05). IL-6 correlated strongly with acute-phase markers and soluble CD163 but not with markers of angiogenesis, YKL-40 or calprotectin. Glucocorticoid treatment down-modulated all markers except for calprotectin and YKL-40. Tissue expression of markers in temporal arteries was confirmed. Conclusion Markers of angiogenesis at baseline and during treatment predict GCA disease course, suggesting utility in patient stratification for glucocorticoid-sparing therapy. Calprotectin and YKL-40 are candidate markers for monitoring vessel wall inflammation. [ABSTRACT FROM AUTHOR]

Published
2019
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104. Circulating CD24 hi CD38 hi regulatory B cells correlate inversely with the Th EM 17 cell frequency in granulomatosis with polyangiitis patients.

Author

Borstel, Anouk von, Lintermans, Lucas L, Heeringa, Peter, Rutgers, Abraham, Stegeman, Coen A, Sanders, Jan Stephan, and Abdulahad, Wayel H

Subjects
TOXIN analysis, NUCLEOTIDE analysis, FLOW cytometry, IN vitro studies, INTERLEUKINS, CARCINOGENS, CELL culture, REGULATORY B cells, GRANULOMATOSIS with polyangiitis, MEMBRANE glycoproteins, T cells
Abstract

Objectives To investigate whether there is a direct relation between expanded proportions of Th17 effector memory (ThEM17) cells and regulatory B cells (Bregs) in peripheral blood of granulomatosis with polyangiitis (GPA) patients. Methods Frequencies of Bregs and ThEM17 cells, as well as ThEM1 cells, were determined by flow cytometry in blood samples from 42 GPA patients in remission and 18 matched healthy controls (HCs). The Breg frequency was defined as CD24hiCD38hiCD19+ cells. ThEM17 cells were defined as CCR6+CXCR3-CCR4+ cells and ThEM1 cells as CCR6-CXCR3+CCR4- cells within the CD3+CD4+CD45RO+CCR7- population. In addition, CD3+CD4+ Th cells from 9 GPA patients were co-cultured in vitro with either total B cells or a Breg-depleted B cell fraction. Cultured cells were stimulated with Staphylococcus Enterotoxin B (SEB) and CpG-oligodeoxynucleotides (CpG-ODN). Th17- (IL-17+) and Th1 cell (IFNγ+) frequencies were determined at baseline and day 5 upon restimulation with phorbol myristate acetate (PMA) and Ca-I. Results A decreased Breg frequency was found in treated GPA patients, whereas an increased ThEM17 cell frequency was observed in treated and untreated GPA patients compared with HCs. Additionally, a decreased ThEM1 cell frequency was seen in untreated GPA patients compared with HCs. In untreated GPA patients circulating Breg frequencies correlated negatively with ThEM17 cells (r = −0.533; P = 0.007) and positively with ThEM1 cells (r = −0.473; P = 0.015). The co-culture experiments revealed a significant increase in the frequency of IL-17+ Th cells in Breg-depleted samples (median: 3%; range: 1–7.5%) compared with Breg-undepleted samples (P = 0.002; undepleted samples median: 2.1%; range: 0.9–6.4%), whereas no difference in the frequency of IFNγ+ Th cells in Breg-depleted cultures was observed (undepleted median: 11.8%; range: 2.8–21% vs Breg-depleted median: 12.2%; range: 2.6–17.6%). Conclusion Bregs modulate ThEM17 responses in GPA patients. Future studies should elaborate on clinical and therapeutical implications of the Breg-Th17 interaction in GPA patients. [ABSTRACT FROM AUTHOR]

Published
2019
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105. Urinary and serum soluble CD25 complements urinary soluble CD163 to detect active renal anti-neutrophil cytoplasmic autoantibody-associated vasculitis: a cohort study.

Author

Dekkema, Gerjan J, Abdulahad, Wayel H, Bijma, Theo, Moran, Sarah M, Ryan, Louise, Little, Mark A, Stegeman, Coen A, Heeringa, Peter, and Sanders, Jan-Stephan F

Subjects
*KIDNEY diseases, *RECEIVER operating characteristic curves, *VASCULITIS, *SERUM, *CREATININE
Abstract

Background Early detection of renal involvement in anti-neutrophil cytoplasmic autoantibody (ANCA)-associated vasculitis (AAV) is of major clinical importance to allow prompt initiation of treatment and limit renal damage. Urinary soluble cluster of differentiation 163 (usCD163) has recently been identified as a potential biomarker for active renal vasculitis. However, a significant number of patients with active renal vasculitis test negative using usCD163. We therefore studied whether soluble CD25 (sCD25), a T cell activation marker, could improve the detection of renal flares in AAV. Methods sCD25 and sCD163 levels in serum and urine were measured by enzyme-linked immunosorbent assay in 72 patients with active renal AAV, 20 with active extrarenal disease, 62 patients in remission and 18 healthy controls. Urinary and blood CD4+ T and CD4+ T effector memory (TEM) cell counts were measured in 22 patients with active renal vasculitis. Receiver operating characteristics (ROC) curves were generated and recursive partitioning was used to calculate whether usCD25 and serum soluble CD25 (ssCD25) add utility to usCD163. Results usCD25, ssCD25 and usCD163 levels were significantly higher during active renal disease and significantly decreased after induction of remission. A combination of usCD25, usCD163 and ssCD25 outperformed all individual markers (sensitivity 84.7%, specificity 95.1%). Patients positive for sCD25 but negative for usCD163 (n  = 10) had significantly higher C-reactive protein levels and significantly lower serum creatinine and proteinuria levels compared with the usCD163-positive patients. usCD25 correlated positively with urinary CD4+ T and CD4+ TEM cell numbers, whereas ssCD25 correlated negatively with circulating CD4+ T and CD4+ TEM cells. Conclusion Measurement of usCD25 and ssCD25 complements usCD163 in the detection of active renal vasculitis. [ABSTRACT FROM AUTHOR]

Published
2019
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109. GIANT CELL ARTERITIS: B CELLS REVISITED

Author

van der Geest, Kornelis S. M., Abdulahad, Wayel H., Horst, Gerda, Roozendaal, Caroline, Rutgers, Abraham, Boots, Annemieke M. H., Brouwer, Elisabeth, Microbes in Health and Disease (MHD), Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), and Translational Immunology Groningen (TRIGR)

Published
2014

114. Urinary Soluble CD163 in Active Renal Vasculitis

Author

O’Reilly, Vincent P., primary, Wong, Limy, additional, Kennedy, Claire, additional, Elliot, Louise A., additional, O’Meachair, Shane, additional, Coughlan, Alice Marie, additional, O’Brien, Eoin C., additional, Ryan, Michelle M., additional, Sandoval, Diego, additional, Connolly, Emma, additional, Dekkema, Gerjan J., additional, Lau, Jiaying, additional, Abdulahad, Wayel H., additional, Sanders, Jan-Stephan F., additional, Heeringa, Peter, additional, Buckley, Colm, additional, O’Brien, Cathal, additional, Finn, Stephen, additional, Cohen, Clemens D., additional, Lindemeyer, Maja T., additional, Hickey, Fionnuala B., additional, O’Hara, Paul V., additional, Feighery, Conleth, additional, Moran, Sarah M., additional, Mellotte, George, additional, Clarkson, Michael R., additional, Dorman, Anthony J., additional, Murray, Patrick T., additional, and Little, Mark A., additional

Published
2016
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115. Are mononuclear cells predominant actors of endothelial damage in vasculitis?

Author

Abdulahad, Wayel H., Silva de Souza, Alexandre W., Kallenberg, Cees G. M., and Translational Immunology Groningen (TRIGR)

Subjects
EXPRESSION, WEGENERS-GRANULOMATOSIS, GLOMERULONEPHRITIS, MEMORY T-CELLS, MICA, ANTINEUTROPHIL CYTOPLASMIC ANTIBODIES, NEUTROPHIL RECRUITMENT, PERIPHERAL-BLOOD, HEALTHY-INDIVIDUALS, DISEASE-ACTIVITY
Published
2013

116. Towards precision medicine in ANCA-associated vasculitis.

Author

Geest, Kornelis S M van der, Brouwer, Elisabeth, Sanders, Jan-Stephan, Sandovici, Maria, Bos, Nicolaas A, Boots, Annemieke M H, Abdulahad, Wayel H, Stegeman, Coen A, Kallenberg, Cees G M, and Heeringa, Peter

Subjects
VASCULITIS treatment, TREATMENT effectiveness, VASCULITIS, INDIVIDUALIZED medicine, ANTINEUTROPHIL cytoplasmic antibodies, SYMPTOMS, GENETICS
Abstract

ANCA-associated vasculitis (AAV) is characterized by inflammation and destruction of small and medium-sized vessels. Current management strategies for AAV have been validated in large groups of patients. However, recent insights indicate that distinct patient subsets may actually exist within AAV, thereby justifying the development of more personalized treatment strategies. In this review, we discuss current evidence for a better classification of AAV based on ANCA type. We describe how thus defined categories of AAV patients may differ in genetic background, clinical presentation, immune pathology, response to treatment and disease outcome. We also explore how these insights may provide a rationale for targeted treatments in different categories of AAV patients. Finally, we provide recommendations on how to further establish precision medicine in AAV. [ABSTRACT FROM AUTHOR]

Published
2018
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118. Intermediate monocytes in ANCA vasculitis: increased surface expression of ANCA autoantigens and IL-1β secretion in response to anti-MPO antibodies

Author

O’Brien, Eóin C., primary, Abdulahad, Wayel H., additional, Rutgers, Abraham, additional, Huitema, Minke G., additional, O’Reilly, Vincent P., additional, Coughlan, Alice M., additional, Harrington, Mark, additional, Heeringa, Peter, additional, Little, Mark A., additional, and Hickey, Fionnuala B., additional

Published
2015
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119. Quantifying Distribution of Flow Cytometric TCR-Vβ Usage with Economic Statistics

Author

van der Geest, Kornelis S. M., primary, Abdulahad, Wayel H., additional, Horst, Gerda, additional, Lorencetti, Pedro G., additional, Bijzet, Johan, additional, Arends, Suzanne, additional, van der Heiden, Marieke, additional, Buisman, Anne-Marie, additional, Kroesen, Bart-Jan, additional, Brouwer, Elisabeth, additional, and Boots, Annemieke M. H., additional

Published
2015
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125. Systematic annotation of celiac disease loci refines pathological pathways and suggests a genetic explanation for increased interferon-gamma levels

Author

Kumar, Vinod, primary, Gutierrez-Achury, Javier, additional, Kanduri, Kartiek, additional, Almeida, Rodrigo, additional, Hrdlickova, Barbara, additional, Zhernakova, Daria V., additional, Westra, Harm-Jan, additional, Karjalainen, Juha, additional, Ricaño-Ponce, Isis, additional, Li, Yang, additional, Stachurska, Anna, additional, Tigchelaar, Ettje F., additional, Abdulahad, Wayel H., additional, Lähdesmäki, Harri, additional, Hofker, Marten H., additional, Zhernakova, Alexandra, additional, Franke, Lude, additional, Lahesmaa, Riitta, additional, Wijmenga, Cisca, additional, and Withoff, Sebo, additional

Published
2014
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132. Serum levels of BAFF, but not APRIL, are increased after rituximab treatment in patients with primary Sjögren's syndrome: data from a placebo-controlled clinical trial

Author

Pollard, Rodney P E, primary, Abdulahad, Wayel H, additional, Vissink, Arjan, additional, Hamza, Nishath, additional, Burgerhof, Johannes G M, additional, Meijer, Jiska M, additional, Visser, Annie, additional, Huitema, Minke G, additional, Spijkervet, Fred K L, additional, Kallenberg, Cees G M, additional, Bootsma, Hendrika, additional, and Kroese, Frans G M, additional

Published
2012
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138. Decreased CXCR1 and CXCR2 expression on neutrophils in anti-neutrophil cytoplasmic autoantibody-associated vasculitides potentially increases neutrophil adhesion and impairs migration

Author

Hu, Nan, primary, Westra, Johanna, additional, Rutgers, Abraham, additional, Doornbos-Van der Meer, Berber, additional, Huitema, Minke G, additional, Stegeman, Coen A, additional, Abdulahad, Wayel H, additional, Satchell, Simon C, additional, Mathieson, Peter W, additional, Heeringa, Peter, additional, and M Kallenberg, Cees G, additional

Published
2011
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141. Low-affinity TCR engagement drives IL-2-dependent post-thymic maintenance of naive CD4+ T cells in aged humans.

Author

Geest, Kornelis S. M., Abdulahad, Wayel H., Teteloshvili, Nato, Tete, Sarah M., Peters, Jorieke H., Horst, Gerda, Lorencetti, Pedro G., Bos, Nicolaas A., Lambeck, Annechien, Roozendaal, Caroline, Kroesen, Bart‐Jan, Koenen, Hans J. P. M., Joosten, Irma, Brouwer, Elisabeth, and Boots, Annemieke M. H.

Subjects
*INTERLEUKIN-2, *T cells, *IMMUNE response, *CELLULAR aging, *HOMEOSTASIS, *LYMPHOID tissue
Abstract

Insight into the maintenance of naive T cells is essential to understand defective immune responses in the context of aging and other immune compromised states. In humans, naive CD4+ T cells, in contrast to CD8+ T cells, are remarkably well retained with aging. Here, we show that low-affinity TCR engagement is the main driving force behind the emergence and accumulation of naive-like CD4+ T cells with enhanced sensitivity to IL-2 in aged humans. In vitro, we show that these CD45 RA+ CD25dim CD4+ T cells can develop from conventional naive CD25− CD4+ T cells upon CD3 cross-linking alone, in the absence of costimulation, rather than via stimulation by the homeostatic cytokines IL-2, IL-7, or IL-15. In vivo, TCR engagement likely occurs in secondary lymphoid organs as these cells were detected in lymph nodes and spleen where they showed signs of recent activation. CD45 RA+ CD25dim CD4+ T cells expressed a broad TCRVβ repertoire and could readily differentiate into functional T helper cells. Strikingly, no expansion of CD45 RA+ CD25dim CD8+ T cells was detected with aging, thereby implying that maintenance of naive CD4+ T cells is uniquely regulated. Our data provide novel insight into the homeostasis of naive T cells and may guide the development of therapies to preserve or restore immunity in the elderly. [ABSTRACT FROM AUTHOR]

Published
2015
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142. Disturbed B Cell Homeostasis in Newly Diagnosed Giant Cell Arteritis and Polymyalgia Rheumatica.

Author

Geest, Kornelis S. M., Abdulahad, Wayel H., Chalan, Paulina, Rutgers, Abraham, Horst, Gerda, Huitema, Minke G., Roffel, Mirjam P., Roozendaal, Caroline, Kluin, Philip M., Bos, Nicolaas A., Boots, Annemieke M. H., and Brouwer, Elisabeth

Subjects
*B cells, *ACADEMIC medical centers, *ENZYME-linked immunosorbent assay, *GIANT cell arteritis, *IMMUNOHISTOCHEMISTRY, *LONGITUDINAL method, *POLYMYALGIA rheumatica, *RESEARCH funding, *STATISTICS, *DATA analysis, *DATA analysis software, *MANN Whitney U Test, *KRUSKAL-Wallis Test, *PHYSIOLOGY
Abstract

Objective. Several lines of evidence indicate that B cells may be involved in the immunopathology of giant cell arteritis (GCA) and polymyalgia rheumatica (PMR). This study was undertaken to examine the distribution of defined B cell subsets, including effector B (Beff) cells and regulatory B (Breg) cells, in patients with GCA and patients with PMR before and after corticosteroid treatment. Methods. Circulating B cells were analyzed in 34 newly diagnosed, untreated patients with GCA or PMR, and in 44 followup samples from patients with GCA or PMR who received corticosteroids for 2 weeks or 3months. For comparison, 40 age-matched healthy controls and 11 rheumatoid arthritis (RA) patients were included. Serum BAFF levels were determined, and temporal arteries were studied by immunohistochemistry. Results. Patients newly diagnosed as having GCA or PMR, but not patients with RA, had decreased numbers of circulating B cells compared to healthy controls. B cell numbers recovered rapidly in treated patients with GCA and PMR in remission. This recovery was not achieved by compensatory hyperproliferation or enhanced bone marrow production. B cell numbers inversely correlated with erythrocyte sedimentation rates, C-reactive protein levels, and serum BAFF levels. Tumor necrosis factor α-positive Beff cells, but not interleukin-10 (IL-10)-positive Breg cells, were decreased in patients newly diagnosed as having GCA or PMR. Following treatment, circulating numbers of Beff cells normalized. The returning Beff cells demonstrated an enhanced capacity to produce IL-6. Few B cells were found in temporal artery biopsy specimens from GCA patients. Conclusion. We show for the first time that the distribution of B cells is highly disturbed in GCA and PMR and that B cells likely contribute to the enhanced IL-6 response in both diseases. [ABSTRACT FROM AUTHOR]

Published
2014
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144. CCR5Δ 32 Genotype Leads to a Th2 Type Directed Immune Response in ESRD Patients.

Author

Muntinghe, Friso L. H., Abdulahad, Wayel H., Huitema, Minke G., Damman, Jeffrey, Seelen, Marc A., Lems, Simon P. M., Hepkema, Bouke G., Navis, Gerjan, and Westra, Johanna

Subjects
*CHRONIC kidney failure, *INFLAMMATION, *IMMUNE response, *T cells, *CYTOKINES, *MORTALITY
Abstract

Background: In patients with end stage renal disease (ESRD) we observed protection from inflammation-associated mortality in CCR5Δ32 carriers, leading to CCR5 deficiency, suggesting impact of CCR5Δ32 on inflammatory processes. Animal studies have shown that CCR5 deficiency is associated with a more pronounced Th2 type immune response, suggesting that in human CCR5Δ32 carriers the immune response may be more Th2 type directed. So, in the present study we determined the Th1-Th2 type directed immune response in ESRD patients carrying and not carrying the CCR5Δ32 genetic variant after stimulation. Methodology/Principal Findings: We tested this hypothesis by determining the levels of IFN-γ and IL-4 and the distribution of Th1, Th2 and Th17 directed circulating CD4+ and CD8+ T cells and regulatory T cells (Tregs) after stimulation in ESRD patients with (n = 10) and without (n = 9) the CCR5Δ32 genotype. The extracellular levels of IFN-γ and IL-4 did not differ between CCR5Δ32 carriers and non carriers. However, based on their intracellular cytokine profile the percentages IL-4 secreting CD4+ and CD8+ T cells carrying the CCR5Δ32 genotype were significantly increased (p = 0.02, respectively p = 0.02) compared to non carriers, indicating a more Th2 type directed response. Based on their intracellular cytokine profile the percentages IFN-γ and IL-17 secreting T cells did not differ between carriers and non-carriers nor did the percentage Tregs, indicating that the Th1, Th17 and T regulatory response was not affected by the CCR5Δ32 genotype. Conclusions/Significance: This first, functional human study shows a more pronounced Th2 type immune response in CCR5Δ32 carriers compared to non carriers. These differences may be involved in the previously observed protection from inflammation-associated mortality in ESRD patients carrying CCR5Δ32. [ABSTRACT FROM AUTHOR]

Published
2012
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145. Immune regulatory mechanisms in ANCA-associated vasculitides

Author

Lepse, Nikola, Abdulahad, Wayel H., Kallenberg, Cees G.M., and Heeringa, Peter

Subjects
*VASCULITIS, *IMMUNOREGULATION, *AUTOANTIBODIES, *NEUTROPHILS, *T cells, *GRANULOMA, *INFLAMMATION
Abstract

Abstract: A group of primary vasculitides is associated with the presence of anti-neutrophil cytoplasmic autoantibodies (ANCA). In these diseases, the contribution of ANCA to disease pathogenesis has been studied extensively. Also, in patients with ANCA-associated vasculitides, the T lymphocyte compartment is dysregulated, as aberrant distribution and function of T cell subsets has been shown. In this review we will discuss the putative role of T lymphocytes in inflammation and granuloma formation, as well as the involvement of B cell compartments in the pathophysiology of ANCA-associated vasculitis. [Copyright &y& Elsevier]

Published
2011
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147. Selective elimination of pathogenic synovial fluid T-cells from Rheumatoid Arthritis and Juvenile Idiopathic Arthritis by targeted activation of Fas-apoptotic signaling

Author

Bremer, Edwin, Abdulahad, Wayel H., de Bruyn, Marco, Samplonius, Douwe F., Kallenberg, Cees G.M., Armbrust, Wineke, Brouwers, E., Wajant, Harald, and Helfrich, Wijnand

Subjects
*SYNOVIAL fluid, *T cells, *APOPTOSIS, *RHEUMATOID arthritis treatment, *GENE expression, *INFLAMMATION, *CELLULAR signal transduction
Abstract

Abstract: In Rheumatoid Arthritis (RA) and Juvenile Idiopathic Arthritis (JIA) elimination of autoreactive T-cells by FasL/Fas-mediated Activation-Induced Cell Death (AICD) appears to be inhibited resulting in the perpetuation of the inflammatory response and concomitant progressive tissue destruction. Here, we report on a novel strategy that aims to overcome the local inhibition of AICD by using rationally designed recombinant fusion proteins in which sFasL is genetically fused to a T-cell selective targeting domain. The series included sFasL fusion proteins with engineered binding specificity for various T-cell surface-expressed proteins including CD7, CD28, RANKL and CD40L. The proposed mode of action is that selective binding of a given sFasL fusion protein results in its accretion at the cell surface of T-cells only, displaying a surplus of sFasL that is available to reactivate AICD in pathogenic synovial T-cells. Of the series of T-cell targeting FasL fusion proteins a CD7-targeted fusion protein, designated scFvCD7:sFasL, proved to be the most potent, with significant pro-apoptotic activity towards synovial fluid T-cells in all patient samples tested (RA; n =22: JIA; n =6). Treatment with scFvCD7:sFasL induced up to 80% apoptosis in CD3-positive synovial T-cells. Importantly, scFvCD7:sFasL potently activated Fas-signaling in synovial TH1-cells as well as synovial Treg cells, but not in synovial TH2 cells. These findings indicate that scFvCD7:sFasL may be of therapeutic value for the selective elimination of pathogenic synovial T-cells of the TH1 subtype in both RA and JIA. [Copyright &y& Elsevier]

Published
2011
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148. Review article: The role of CD4+ T cells in ANCA-associated systemic vasculitis.

Author

Abdulahad, Wayel H., Stegeman, Coen A., and Kallenberg, Cees G. M.

Subjects
*CD4 antigen, *VASCULITIS, *T cells, *PROTEINASES, *IMMUNOGLOBULINS
Abstract

Antineutrophil cytoplasmic autoantibody (ANCA)-associated systemic vasculitis (AASV) constitutes a group of primary vasculitides associated with antineutrophil cytoplasmic autoantibodies, which are either directed to proteinase-3 or myeloperoxidase. In contrast to other forms of vasculitis, immuohistologic evaluation of affected tissues in patients with AASV, particularly the kidneys, demonstrated an absence or paucity of immunoglobulins, which could suggest involvement of cell-mediated injury in this disorder. Several studies have shed light on T cell-mediated immune responses playing a role in the pathophysiology of AASV. Imbalance of CD4+ T-cell subsets has been demonstrated in the peripheral blood of patients with AASV. The trigger that leads to this imbalance remains to be defined, but clinical evidence shows that nasal carriage of Staphylococcus aureus constitutes a risk factor for disease exacerbation. Recent data show that superantigens and peptidoglycans from these Gram-positive bacteria can induce skewing of T-cell responses towards pathogenic interleukin (IL)-17-producing T-helper cells (Th17). Overproduction of IL-17 in response to this infection might aggravate inflammatory responses and contribute to the production of autoantibodies as well as to granuloma formation and tissue injury in patients with AASV. Next to Th17 cells, memory CD4+ T cells with the effector cytotoxic phenotype (CD4+ TEM) have also been demonstrated to constitute a major effector pathway of tissue injury in patients with pauci-immune glomerulonephritis. Therefore, future perspectives for treatment of AASV could be built on neutralization of IL-17 and depletion of CD4+ TEM cells. [ABSTRACT FROM AUTHOR]

Published
2009
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149. research paper CD27-triggering on primary plasma cell leukaemia cells has anti-apoptotic effects involving mitogen activated protein kinases.

Author

Guikema, Jeroen E.J., Vellenga, Edo, Abdulahad, Wayel H., Hovenga, Sjoerd, and Bos, Nicolaas A.

Subjects
PLASMA cell leukemia, PLASMA cells, LEUKEMIA, HEMATOLOGY, THERAPEUTICS
Abstract

Primary plasma cell leukaemia (PCL) is a rare plasma cell malignancy, which is related to multiple myeloma (MM) and is characterized by a poor prognosis. In a previous study we demonstrated that PCL plasma cells display a high expression of CD27, in contrast to MM plasma cells. The present study was set out to assess the functional properties of CD27 expressed on PCL plasma cells by triggering with its ligand CD70. Using CD27-expressing purified plasma cells from a PCL patient we demonstrated that CD27-triggering modestly inhibited spontaneous and dexamethasone-induced apoptosis. In vitro stimulation and Western blotting showed that activation of p38 and extracellular-regulated kinase 1/2 (ERK1/2) mitogen-activated protein kinases (MAPK) was associated with CD27-mediated signal transduction. Specific inhibition of p38 and ERK1/2 MAPK abolished the anti-apoptotic effects of CD27-triggering. Interestingly, simultaneous inhibition of p38 and ERK1/2 strongly sensitized PCL cells for dexamethasone-induced apoptosis. Finally, in dexamethasone-treated PCL cells, CD27-triggering was associated with persistent DNA-binding activity of activator protein 1 (AP-1) but not of nuclear factor- κB. These findings suggest that, in primary PCL, specific anti-apoptotic pathways exist that might provide novel therapeutic targets. [ABSTRACT FROM AUTHOR]

Published
2004
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150. Pathogenesis of ANCA-Associated Vasculitis: New Possibilities for Intervention

Author

Kallenberg, Cees G.M., Stegeman, Coen A., Abdulahad, Wayel H., and Heeringa, Peter

Abstract

The antineutrophil cytoplasmic antibody (ANCA)-associated vasculitides (AAVs) comprise granulomatosis with polyangiitis (GPA), primarily associated with antibodies to proteinase 3 (PR3-ANCA); microscopic polyangiitis (MPA); and eosinophilic granulomatosis with polyangiitis (EGPA), both principally associated with antibodies to myeloperoxidase (MPO-ANCA). Genetic and environmental factors are involved in their etiopathogenesis, with a possible role for silica exposure in AAVs and Staphylococcus aureusinfection in GPA. The distinct associations of PR3-ANCA and MPO-ANCA with different HLA class II antigens, which are stronger than those with the associated diseases, suggest a pathogenic role for those ANCAs and indicate that GPA and MPA are different diseases. Both in vitro and in vivo experimental data have shown that MPO-ANCA can induce necrotizing small-vessel vasculitis and glomerulonephritis. The additional role of the alternative pathway of complement activation has been demonstrated in human and experimental pathology. Also, T cells seem to be involved in lesion development, particularly in the kidney. Granuloma formation, as seen in PR3-ANCA–associated GPA, is not well explained by the presence of autoantibodies in experimental models. Here, T cells seem crucial. Recently obtained insights into the pathogenesis of AAVs have led to more targeted treatment of these life-threatening diseases.

Published
2013
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