Your search keyword '"van Bergen, Jeroen"' showing total 10 results

1. Local Communication Among Mucosal Immune Cells in Patients With Celiac Disease.

Author

van Bergen, Jeroen, Mulder, Chris J., Mearin, M. Luisa, and Koning, Frits

Abstract

In patients with celiac disease, gluten consumption causes inflammation of the duodenum, and, to a lesser extent, the proximal jejunum. Immune-dominant gluten peptides are modified by the enzyme TG2, leading to their high-affinity binding to HLA-DQ2 or HLA-DQ8 molecules, present in people with a predisposition to celiac disease. Gluten peptide−loaded HLA-DQ2 or HLA-DQ8 molecules are recognized by highly conserved receptors on CD4 + T cells in the lamina propria. B cells specific for TG2 and modified gluten peptides are also abundant in the lamina propria of patients with celiac disease. In the epithelium, interleukin-15 activates intraepithelial lymphocytes that promote destruction of epithelial cells. However, it is not clear how the immune responses in the lamina propria and the epithelium, separated by a basement membrane, are linked. We review the immune processes that occur in the lamina propria and their potential effects on epithelial pathology in celiac disease. [ABSTRACT FROM AUTHOR]

Published

2015

2. Sa1772 Ilc-Like Lymphomas in Refractory Celiac Disease Type II Respond to Multiple Common γ-Chain Cytokines and Are Sensitive to JAK-Inhibitors.

Author

Kooy-Winkelaar, Yvonne, Schmitz, Frederike, Mearin, M. Luisa, Bouma, Gerd, Mulder, Chris J., Koning, Frits, and van Bergen, Jeroen

Published

2015

3. 54-OR: KIR-ligand mismatches are associated with reduced long-term graft survival in HLA fully compatible kidney transplantation

Author

van Bergen, Jeroen, Thompson, Alan, Haasnoot, Geert W., Roodnat, Joke J., de Fijter, Johan W., Claas, Frans H.J., Koning, Frits, and Doxiadis, Ilias I.N.

Published

2011

4. 379 Can Prolyl Endoprotease Enzyme Treatment Mitigate the Toxic Effect of Gluten in Coeliac Patients?

Author

Tack, Greetje J., van de Water, Jolanda M., Kooy-Winkelaar, E.M., van Bergen, Jeroen, Meijer, Gerrit A., von Blomberg, Boudewina M., Schreurs, Marco W., Bruins, Maaike J., Edens, Luppo, Mulder, Chris J., and Koning, Frits

Published

2010

5. Dendritic cells promote expansion and survival of aberrant TCR-negative intraepithelial lymphocyte lines from refractory celiac disease type II patients.

Author

Schmitz, Frederike, Tjon, Jennifer M.-L., van Bergen, Jeroen, and Koning, Frits

Subjects

*DENDRITIC cells, *T cell receptors, *LYMPHOCYTES, *CELIAC disease, *CELL proliferation, *APOPTOSIS inhibition

Abstract

Highlights: [•] TCR-negative IEL lines are derived from refractory celiac disease II patients. [•] Dendritic cells (DCs) induce proliferation and inhibit apoptosis of such RCDII lines. [•] DC-induced proliferation of RCDII lines is independent of IL-15 or HLA genotype. [•] IFNγ and CXCL10 is produced by cocultures of DC and RCDII lines. [•] DC may therefore contribute to uncontrolled expansion of RCDII cells in vivo. [ABSTRACT FROM AUTHOR]

Published

2014

6. KIR-HLA intercourse in HIV disease

Author

Carrington, Mary, Martin, Maureen P., and van Bergen, Jeroen

Subjects

*HIV infections, *KILLER cells, *HLA histocompatibility antigens, *IMMUNOCOMPETENT cells, *IMMUNE response, *MICROBIAL virulence, *PATHOGENIC microorganisms

Abstract

Human leukocyte antigen (HLA) class I loci are essential to an effective immune response against a wide variety of pathogenic microorganisms, and they represent the prototypes for genetic polymorphism that are sustained through balancing selection. The functional significance of HLA class I variation is better exemplified by studies involving HIV type 1 (HIV-1) than any other infectious organism. HLA class I molecules are essential to the acquired immune response, but they are also important in innate immunity as ligands for the killer cell immunoglobulin-like receptors (KIR), which modulate natural killer cell activity. Here we concentrate on the interaction between the HLA-B and KIR3DL1/KIR3DS1 genes, describe the effects of these loci on HIV disease, and discuss questions that remain unresolved. [Copyright &y& Elsevier]

Published

2008

7. Pyroptosis-inducing active caspase-1 as a genetic adjuvant in anti-cancer DNA vaccination.

Author

Arakelian, Tsolere, Oosterhuis, Koen, Tondini, Elena, Los, Mandy, Vree, Jana, van Geldorp, Mariska, Camps, Marcel, Teunisse, Bram, Zoutendijk, Iris, Arens, Ramon, Zondag, Gerben, Ossendorp, Ferry, and van Bergen, Jeroen

Subjects

*CASPASES, *DNA, *DNA vaccines, *CELL death, *VACCINATION, *PROGRAMMED cell death 1 receptors, *OVALBUMINS

Abstract

Pyroptosis is a recently discovered form of inflammatory programmed necrosis characterized by caspase-1-mediated and gasdermin D-dependent cell death leading to the release of pro-inflammatory cytokines such as Interleukin-1 beta (IL-1β). Here, we evaluated whether pyroptosis could be exploited in DNA vaccination by incorporating a constitutively active variant of caspase-1 to the antigen-expressing DNA. In vitro , transfection with constitutively active caspase-1 DNA induced pro-IL-1β maturation and IL-1β release as well as gasdermin D-dependent cell death. To test active caspase-1 as a genetic adjuvant for the induction of antigen-specific T cell responses, mice were vaccinated intradermally with a DNA vaccine consisting of the active caspase-1 plasmid together with a plasmid encoding an ovalbumin-derived CD8 T cell epitope. Active caspase-1 accelerated and amplified antigen-specific CD8 T cell responses when administered simultaneously with the DNA vaccine at an equimolar dose. Moreover, upon challenge with melanoma cells expressing ovalbumin, mice vaccinated with the antigen vaccine adjuvanted with active caspase-1 showed significantly better survival compared to the non-adjuvanted group. In conclusion, we have developed a novel genetic adjuvant that for the first time employs the pyroptosis pathway to improve DNA vaccination against cancer. [ABSTRACT FROM AUTHOR]

Published

2022

8. Diverse T Cell Receptor Gene Usage in HLA-DQ8-Associated Celiac Disease Converges into a Consensus Binding Solution.

Author

Petersen, Jan, Kooy-Winkelaar, Yvonne, Loh, Khai Lee, Tran, Mai, van Bergen, Jeroen, Koning, Frits, Rossjohn, Jamie, and Reid, Hugh H.

Subjects

*T cell receptors, *HLA histocompatibility antigens, *CELIAC disease, *BINDING agents, *CRYSTAL structure

Abstract

Summary In HLA-DQ8-associated celiac disease, TRAV26-2 + -TRBV9 + and TRAV8-3 + -TRBV6 + T cells recognize the immunodominant DQ8-glia-α1 epitope, whereupon a non-germline-encoded arginine residue played a key role in binding HLA-DQ8-glia-α1. Whether distinct T cell receptor (TCR) recognition modes exist for gliadin epitopes remains unclear. TCR repertoire analysis revealed populations of HLA-DQ8-glia-α1 and HLA-DQ8.5-glia-γ1 restricted TRAV20 + -TRBV9 + T cells that did not possess a non-germline-encoded arginine residue. The crystal structures of a TRAV20 + -TRBV9 + TCR-HLA-DQ8-glia-α1 complex and two TRAV20 + -TRBV9 + TCR-HLA-DQ8.5-glia-γ1 complexes were determined. This revealed that the differential specificity toward DQ8-glia-α1 and DQ8.5-glia-γ1 was governed by CDR3β-loop-mediated interactions. Surprisingly, a germline-encoded arginine residue within the CDR1α loop of the TRAV20 + TCR substituted for the role of the non-germline-encoded arginine in the TRAV26-2 + -TRBV9 + and TRAV8-3 + -TRBV6 + TCRs. Thus, in celiac disease, the responding TCR repertoire is driven by a common mechanism that selects for structural elements within the TCR that have convergent binding solutions in HLA-DQ8-gliadin recognition. [ABSTRACT FROM AUTHOR]

Published

2016

9. Origin and immunophenotype of aberrant IEL in RCDII patients

Author

Tack, Greetje J., van Wanrooij, Roy L.J., Langerak, Anton W., Tjon, Jennifer M.L., von Blomberg, B. Mary E., Heideman, Danielle A.M., van Bergen, Jeroen, Koning, Frits, Bouma, Gerd, Mulder, Chris J.J., and Schreurs, Marco W.J.

Subjects

*IMMUNOPHENOTYPING, *LYMPHOCYTES, *CELIAC disease, *T-cell lymphoma, *T-cell receptor genes, *CELL populations, *PATIENTS

Abstract

Abstract: Objectives: Aberrant intra-epithelial lymphocytes (IELs) are the hallmark of refractory coeliac disease type II RCDII and considered a premalignant cell population from which aggressive enteropathy-associated T cell lymphoma (EATL) can evolve. The aim of this study was to gain further insight in the origin and characteristics of aberrant IELs by analysing T-cell receptor (TCR) rearrangements, and by immunophenotypic analysis of aberrant IELs. Design: Duodenal biopsies from 18 RCDII patients and three RCDII cell lines were analysed for the presence of TCR delta, gamma, and beta rearrangements. In addition, IELs isolated from biopsies derived from RCDII patients were phenotypically analysed. Results: Aberrant IELs showed an upregulated expression of granzyme B and decreased expression of PCNA. TCR rearrangements in the aberrant IEL population in biopsies of RCDII patients were heterogenic, which is most likely due to a variation in maturity. Similarly, RCDII cell lines displayed a heterogenic TCR rearrangement pattern. Conclusion: Aberrant IELs originate from deranged immature T lymphocytes and display clear differentiation to a cytotoxic phenotype. Aberrant IELs displayed different stages of maturity between RCDII patients, of which only the patients harbouring the most mature aberrant IEL population developed an EATL. [Copyright &y& Elsevier]

Published

2012

10. 43-OR: Evidence for Natural Killer Cell Induced Graft Loss in HLA Full Compatible Kidney Transplantation

Author

Doxiadis, Ilias I.N., Thompson, Allan, Haasnot, Geert W., Roodnat, Joke I., de Fijter, Johan W., Claas, Frans H.J., Koning, Fritz, and van Bergen, Jeroen

Published

2010