Your search keyword '"van Helden PM"' showing total 22 results

1. Leveraging Vγ9Vδ2 T cells against prostate cancer through a VHH-based PSMA-Vδ2 bispecific T cell engager.

Author

King LA, Veth M, Iglesias-Guimarais V, Blijdorp I, Kloosterman J, Vis AN, Roovers RC, Hulsik DL, Riedl T, Adang AEP, Parren PWHI, van Helden PM, de Gruijl TD, and van der Vliet HJ

Abstract

Vγ9Vδ2 T cells constitute a homogeneous effector T cell population that lyses tumors of different origin, including the prostate. We generated a bispecific T cell engager (bsTCE) to direct Vγ9Vδ2 T cells to PSMA + prostate cancer (PCa) cells. The PSMA-Vδ2 bsTCE triggered healthy donor and PCa patient-derived Vγ9Vδ2 T cells to lyse PSMA + PCa cell lines and patient-derived tumor cells while sparing normal prostate cells and enhanced Vγ9Vδ2 T cell antigen cross-presentation to CD8 + T cells. Vγ9Vδ2 T cell expressed NKG2D and DNAM-1 contributed to Vγ9Vδ2 T cell activation and tumor lysis at low PSMA-Vδ2 bsTCE concentrations. In vivo models confirmed the antitumor efficacy of the bsTCE and demonstrated a half-life of 6-7 days. Tissue-cross reactivity analysis was in line with known tissue distribution of PSMA and Vγ9Vδ2 T cells. Together these data show the PSMA-Vδ2 bsTCE to represent a promising anti-tumor strategy and supports its ongoing evaluation in a phase 1/2a clinical trial in therapy refractory metastatic castration-resistant PCa., Competing Interests: L.A.K., M.V.,and J.K. are/were funded by Lava Therapeutics NV. T.R., R.C.R., A.E.P.A., P.W.H.I.P., T.D.d.G.,and H.J.v.d.V. own Lava Therapeutics NV shares. V.I.-G., I.B., R.C.R., D.L.H., T.R., A.E.P.A., P.W.H.I.P., and H.J.v.d.V. are/were employees of Lava Therapeutics NV. T.D.d.G.is scientific advisor to Lava Therapeutics NV. Patent registration related to this work: Antibodies that bind PSMA and gamma-delta T cell receptors, Lava Therapeutics NV, WO2022008646A1, 2022-01-13., (© 2024 The Authors.)

Published

2024

2. Vδ2 T-cell engagers bivalent for Vδ2-TCR binding provide anti-tumor immunity and support robust Vγ9Vδ2 T-cell expansion.

Author

King LA, de Jong M, Veth M, Lutje Hulsik D, Yousefi P, Iglesias-Guimarais V, van Helden PM, de Gruijl TD, and van der Vliet HJ

Abstract

Background: Vγ9Vδ2 T-cells are antitumor immune effector cells that can detect metabolic dysregulation in cancer cells through phosphoantigen-induced conformational changes in the butyrophilin (BTN) 2A1/3A1 complex. In order to clinically exploit the anticancer properties of Vγ9Vδ2 T-cells, various approaches have been studied including phosphoantigen stimulation, agonistic BTN3A-specific antibodies, adoptive transfer of expanded Vγ9Vδ2 T-cells, and more recently bispecific antibodies. While Vγ9Vδ2 T-cells constitute a sizeable population, typically making up ~1-10% of the total T cell population, lower numbers have been observed with increasing age and in the context of disease., Methods: We evaluated whether bivalent single domain antibodies (VHHs) that link Vδ2-TCR specific VHHs with different affinities could support Vγ9Vδ2 T-cell expansion and could be incorporated in a bispecific engager format when additionally linked to a tumor antigen specific VHH., Results: Bivalent VHHs that link a high and low affinity Vδ2-TCR specific VHH can support Vγ9Vδ2 T-cell expansion. The majority of Vγ9Vδ2 T-cells that expanded following exposure to these bivalent VHHs had an effector or central memory phenotype and expressed relatively low levels of PD-1. Bispecific engagers that incorporated the bivalent Vδ2-TCR specific VHH as well as a tumor antigen specific VHH triggered antitumor effector functions and supported expansion of Vγ9Vδ2 T-cells in vitro and in an in vivo model in NOG-hIL-15 mice., Conclusion: By enhancing the number of Vγ9Vδ2 T-cells available to exert antitumor effector functions, these novel Vδ2-bivalent bispecific T cell engagers may promote the overall efficacy of bispecific Vγ9Vδ2 T-cell engagement, particularly in patients with relatively low levels of Vγ9Vδ2 T-cells., Competing Interests: NV. TG and HV own LAVA Therapeutics NV shares. DH, PY, VI-G, PH and HV are/were employed by LAVA Therapeutics NV. TG is scientific advisor to LAVA Therapeutics NV. The authors declare that this study received funding from Lava Therapeutics NV. LK, MJ and MV were funded by LAVA Therapeutics NV., (Copyright © 2024 King, de Jong, Veth, Lutje Hulsik, Yousefi, Iglesias-Guimarais, van Helden, de Gruijl and van der Vliet.)

Published

2024

3. Combinatorial multimer staining and spectral flow cytometry facilitate quantification and characterization of polysaccharide-specific B cell immunity.

Author

Hoving D, Marques AHC, Huisman W, Nosoh BA, de Kroon AC, van Hengel ORJ, Wu BR, Steenbergen RAM, van Helden PM, Urban BC, Dhar N, Ferreira DM, Kwatra G, Hokke CH, and Jochems SP

Subjects

Flow Cytometry, Polysaccharides, Bacterial, Immunity, Immunization, Vaccines

Abstract

Bacterial capsular polysaccharides are important vaccine immunogens. However, the study of polysaccharide-specific immune responses has been hindered by technical restrictions. Here, we developed and validated a high-throughput method to analyse antigen-specific B cells using combinatorial staining with fluorescently-labelled capsular polysaccharide multimers. Concurrent staining of 25 cellular markers further enables the in-depth characterization of polysaccharide-specific cells. We used this assay to simultaneously analyse 14 Streptococcus pneumoniae or 5 Streptococcus agalactiae serotype-specific B cell populations. The phenotype of polysaccharide-specific B cells was associated with serotype specificity, vaccination history and donor population. For example, we observed a link between non-class switched (IgM + ) memory B cells and vaccine-inefficient S. pneumoniae serotypes 1 and 3. Moreover, B cells had increased activation in donors from South Africa, which has high-incidence of S. agalactiae invasive disease, compared to Dutch donors. This assay allows for the characterization of heterogeneity in B cell immunity that may underlie immunization efficacy., (© 2023. The Author(s).)

Published

2023

4. Modulating the microenvironment during FVIII uptake influences the nature of FVIII-peptides presented by antigen-presenting cells.

Author

Lubich C, Steinitz KN, Hoelbl B, Prenninger T, van Helden PM, Weiller M, and Reipert BM

Subjects

Humans, Mice, Animals, Factor VIII, CD4-Positive T-Lymphocytes, Antigen-Presenting Cells, Peptides, Hemophilia A drug therapy, Hemostatics

Abstract

Background and Aims: Hemophilia A is a severe bleeding disorder caused by the deficiency of functionally active coagulation factor VIII (FVIII). The induction of neutralizing anti-drug antibodies is a major complication in the treatment of hemophilia A patients with FVIII replacement therapies. Why some patients develop neutralizing antibodies (FVIII inhibitors) while others do not is not well understood. Previous studies indicated that the induction of FVIII inhibitors requires cognate interactions between FVIII-specific B cells and FVIII-specific CD4+ T cells in germinal center reactions. In this study, we investigated the FVIII peptide repertoire presented by antigen-presenting cells (APCs) under different microenvironment conditions that are expected to alter the uptake of FVIII by APCs. The aim of this study was to better understand the association between different microenvironment conditions during FVIII uptake and the FVIII peptide patterns presented by APCs., Methods: We used a FVIII-specific CD4+ T cell hybridoma library derived from humanized HLA-DRB1*1501 (human MHC class II) hemophilic mice that were treated with human FVIII. APCs obtained from the same mouse strain were preincubated with FVIII under different conditions which are expected to alter the uptake of FVIII by APCs. Subsequently, these preincubated APCs were used to stimulate the FVIII-specific CD4+ T cell hybridoma library. Stimulation of peptide-specific CD4+ T-cell hybridoma clones was assessed by analyzing the IL-2 release into cell culture supernatants., Results: The results of this study indicate that the specific microenvironment conditions during FVIII uptake by APCs determine the peptide specificities of subsequently activated FVIII-specific CD4+ T cell hybridoma clones. Incubation of APCs with FVIII complexed with von Willebrand Factor, FVIII activated by thrombin or FVIII combined with a blockade of receptors on APCs previously associated with FVIII uptake and clearance, resulted in distinct peptide repertoires of subsequently activated hybridoma clones., Conclusion: Based on our data we conclude that the specific microenvironment during FVIII uptake by APCs determines the FVIII peptide repertoire presented on MHC class II expressed by APCs and the peptide specificity of subsequently activated FVIII-specific CD4+ T cell hybridoma clones., Competing Interests: MW is an employee of Baxalta Innovations GmbH, a member of the Takeda group of companies, Vienna, Austria. CL, KS, BH, TP, PH, and BR were employees of Baxalta Innovations GmbH, a member of the Takeda group of companies, Vienna, Austria, at the time when this study was done. The authors declare that this study received funding from Baxalta Innovations GmbH. The funder had the following involvement in the study: study design, interpretation of data, writing of this article and the decision to submit it for publication., (Copyright © 2022 Lubich, Steinitz, Hoelbl, Prenninger, van Helden, Weiller and Reipert.)

Published

2022

5. Melanoma cells can be eliminated by sialylated CD43 × CD3 bispecific T cell engager formats in vitro and in vivo.

Author

de Jong G, Bartels L, Kedde M, Verdegaal EME, Gillissen MA, Levie SE, Cercel MG, van Hal-van Veen SE, Fatmawati C, van de Berg D, Yasuda E, Claassen YB, Bakker AQ, van der Burg SH, Schotte R, Villaudy J, Spits H, Hazenberg MD, van Helden PM, and Wagner K

Subjects

Animals, Apoptosis, Cell Proliferation, Cytotoxicity, Immunologic, Female, Humans, In Vitro Techniques, Melanoma immunology, Melanoma pathology, Mice, Mice, Inbred NOD, Mice, SCID, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Antibodies, Bispecific pharmacology, Antibodies, Monoclonal pharmacology, Antineoplastic Agents, Immunological pharmacology, CD3 Complex immunology, Leukosialin immunology, Melanoma therapy, N-Acetylneuraminic Acid chemistry, T-Lymphocytes immunology

Abstract

Targeted cancer therapy with monoclonal antibodies has proven successful for different cancer types but is limited by the availability of suitable antibody targets. CD43s, a unique sialylated form of CD43 expressed by hematologic malignancies, is a recently identified target and antibodies interacting with CD43s may have therapeutic potential against acute myeloid leukemia (AML) and myelodysplastic syndrome. CD43s is recognized by the human antibody AT1413, that was derived from a high-risk AML patient who successfully cleared leukemia after allogeneic stem cell transplantation. Here we observed that AT1413 binds also to certain non-hematopoietic tumor cells, particularly melanoma and breast cancer. AT1413 immune precipitated CD43s from melanoma cells confirming that it recognizes the same target on melanoma as on AML. AT1413 induced antibody-dependent cellular cytotoxicity against short-term cultured patient-derived melanoma samples. However, AT1413 was unable to affect the growth of melanoma cells in vivo. To increase the efficacy of AT1413 as a therapeutic antibody, we generated two different formats of bispecific T-cell engaging antibodies (TCEs): one binding bivalently (bTCE) and the other monovalently (knob-in-hole; KiH) to both CD43s and CD3ε. In vitro, these TCEs redirected T-cell cytotoxicity against melanoma cells with differences in potencies. To investigate their effects in vivo, we grafted mice that harbor a human immune system with the melanoma cell line A375. Treatment with both AT1413 bTCE and AT1413 KiH significantly reduced tumor outgrowth in these mice. These data indicate a broad therapeutic potential of AT1413 that includes AML and CD43s-expressing solid tumors that originate from CD43-negative tissues.

Published

2021

6. A Chemo-enzymatically Linked Bispecific Antibody Retargets T Cells to a Sialylated Epitope on CD43 in Acute Myeloid Leukemia.

Author

Bartels L, de Jong G, Gillissen MA, Yasuda E, Kattler V, Bru C, Fatmawati C, van Hal-van Veen SE, Cercel MG, Moiset G, Bakker AQ, van Helden PM, Villaudy J, Hazenberg MD, Spits H, and Wagner K

Subjects

Animals, Apoptosis, Cell Proliferation, Cytotoxicity, Immunologic, Endothelial Cells drug effects, Endothelial Cells immunology, Endothelial Cells metabolism, Epitopes drug effects, Epitopes metabolism, Female, Humans, Leukemia, Myeloid, Acute immunology, Leukemia, Myeloid, Acute metabolism, Leukemia, Myeloid, Acute pathology, Leukocytes, Mononuclear drug effects, Leukocytes, Mononuclear immunology, Leukocytes, Mononuclear metabolism, Lymphocyte Activation drug effects, Mice, Mice, Inbred NOD, Mice, SCID, Prognosis, T-Lymphocytes drug effects, T-Lymphocytes metabolism, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Antibodies, Bispecific pharmacology, Epitopes immunology, Leukemia, Myeloid, Acute drug therapy, Leukosialin immunology, Lymphocyte Activation immunology, N-Acetylneuraminic Acid metabolism, T-Lymphocytes immunology

Abstract

Acute myeloid leukemia (AML) is a high-risk disease with a poor prognosis, particularly in elderly patients. Because current AML treatment relies primarily on untargeted therapies with severe side effects that limit patient eligibility, identification of novel therapeutic AML targets is highly desired. We recently described AT1413, an antibody produced by donor B cells of a patient with AML cured after allogeneic hematopoietic stem cell transplantation. AT1413 binds CD43s, a unique sialylated epitope on CD43, which is weakly expressed on normal myeloid cells and overexpressed on AML cells. Because of its selectivity for AML cells, we considered CD43s as a target for a bispecific T-cell-engaging antibody (bTCE) and generated a bTCE by coupling AT1413 to two T-cell-targeting fragments using chemo-enzymatic linkage. In vitro , AT1413 bTCE efficiently induced T-cell-mediated cytotoxicity toward different AML cell lines and patient-derived AML blasts, whereas endothelial cells with low binding capacity for AT1413 remained unaffected. In the presence of AML cells, AT1413 bTCE induced upregulation of T-cell activation markers, cytokine release, and T-cell proliferation. AT1413 bTCE was also effective in vivo . Mice either coinjected with human peripheral blood mononuclear cells or engrafted with human hematopoietic stem cells [human immune system (HIS) mice] were inoculated with an AML cell line or patient-derived primary AML blasts. AT1413 bTCE treatment strongly inhibited tumor growth and, in HIS mice, had minimal effects on normal human hematopoietic cells. Taken together, our results indicate that CD43s is a promising target for T-cell-engaging antibodies and that AT1413 holds therapeutic potential in a bTCE-format. SIGNIFICANCE: These findings offer preclinical evidence for the therapeutic potential of a bTCE antibody that targets a sialylated epitope on CD43 in AML., (©2019 American Association for Cancer Research.)

Published

2019

7. AML-specific cytotoxic antibodies in patients with durable graft-versus-leukemia responses.

Author

Gillissen MA, Kedde M, Jong G, Moiset G, Yasuda E, Levie SE, Bakker AQ, Claassen YB, Wagner K, Böhne M, Hensbergen PJ, Speijer D, van Helden PM, Beaumont T, Spits H, and Hazenberg MD

Subjects

Adult, Animals, Combined Modality Therapy, Female, Hematopoietic Stem Cell Transplantation, Humans, Leukemia, Myeloid, Acute pathology, Leukemia, Myeloid, Acute therapy, Male, Mice, SCID, Middle Aged, Prognosis, Antibodies, Monoclonal therapeutic use, Apoptosis immunology, Graft vs Leukemia Effect immunology, Killer Cells, Natural immunology, Leukemia, Myeloid, Acute immunology, Ribonucleoprotein, U5 Small Nuclear immunology, T-Lymphocytes, Cytotoxic immunology

Abstract

Most patients with acute myeloid leukemia (AML) can only be cured when allogeneic hematopoietic stem-cell transplantation induces a graft-versus-leukemia immune response (GVL). Although the role of T cells and natural killer cells in tumor immunology has been established, less is known about the contribution of B cells. From B cells of high-risk patients with AML with potent and lasting GVL responses, we isolated monoclonal antibodies directed against antigens expressed on the cell surface of AML cells but not on normal hematopoietic and nonhematopoietic cells. A number of these donor-derived antibodies recognized the U5 snRNP200 complex, a component of the spliceosome that in normal cells is found in the cell. In AML however, the U5 snRNP200 complex is exposed on the cell membrane of leukemic blasts. U5 snRNP200 complex-specific antibodies induced death of AML cells in an Fc receptor-dependent way in the absence of cytotoxic leukocytes or complement. In an AML mouse model, treatment with U5 snRNP200 complex-specific antibodies led to significant tumor growth inhibition. Thus, donor-derived U5 snRNP200 complex-recognizing AML-specific antibodies may contribute to antitumor responses., (© 2018 by The American Society of Hematology.)

Published

2018

8. Patient-derived antibody recognizes a unique CD43 epitope expressed on all AML and has antileukemia activity in mice.

Author

Gillissen MA, de Jong G, Kedde M, Yasuda E, Levie SE, Moiset G, Hensbergen PJ, Bakker AQ, Wagner K, Villaudy J, van Helden PM, Spits H, and Hazenberg MD

Abstract

Immunotherapy has proven beneficial in many hematologic and nonhematologic malignancies, but immunotherapy for acute myeloid leukemia (AML) and myelodysplastic syndrome (MDS) is hampered by the lack of tumor-specific targets. We took advantage of the tumor-immunotherapeutic effect of allogeneic hematopoietic stem cell transplantation and searched the B-cell repertoire of a patient with a lasting and potent graft-versus-AML response for the presence of AML-specific antibodies. We identified an antibody, AT1413, that was of donor origin and that specifically recognizes a novel sialylated epitope on CD43 (CD43s). Strikingly, CD43s is expressed on all World Health Organization 2008 types of AML and MDS. AT1413 induced antibody-dependent cell-mediated cytotoxicity and complement-dependent cytotoxicity of AML cells in vitro. Of note, AT1413 was highly efficacious against AML cells in a humanized mouse model without affecting nonmalignant human myeloid cells, suggesting AT1413 has potential as a therapeutic antibody., Competing Interests: Conflict-of-interest disclosure: M.A.G., G.d.J., M.K., E.Y., S.E.L., G.M., A.Q.B., K.W., J.V., P.M.v.H., and H.S. are employees of AIMM Therapeutics, a company that develops monoclonal antibodies for prevention and treatment of infectious diseases and cancer.

Published

2017

9. AML relapse after rituximab treatment for GvHD: crucial role for B cells in GvL responses.

Author

Gillissen MA, de Jong G, Levie SE, Yasuda E, Bakker AQ, Evers LM, Pals ST, Huisman C, van Helden PM, Spits H, and Hazenberg MD

Subjects

Adult, B-Lymphocytes immunology, B-Lymphocytes physiology, Fatal Outcome, Graft vs Host Disease etiology, Graft vs Leukemia Effect drug effects, Hematopoietic Stem Cell Transplantation adverse effects, Humans, Leukemia, Myeloid, Acute complications, Leukemia, Myeloid, Acute therapy, Male, Recurrence, Transplantation, Homologous, Graft vs Host Disease drug therapy, Leukemia, Myeloid, Acute pathology, Rituximab adverse effects

Published

2016

10. The modified FACS calcein AM retention assay: A high throughput flow cytometer based method to measure cytotoxicity.

Author

Gillissen MA, Yasuda E, de Jong G, Levie SE, Go D, Spits H, van Helden PM, and Hazenberg MD

Subjects

Biological Assay, Cell Line, Tumor, Cell Survival, Fluorescent Dyes chemistry, Humans, Rituximab chemistry, Trastuzumab chemistry, Tumor Cells, Cultured, Cytotoxicity, Immunologic, Flow Cytometry methods, Fluoresceins chemistry, Killer Cells, Natural immunology

Abstract

Current methods to determine cellular cytotoxicity in vitro are hampered by background signals that are caused by auto-fluorescent target and effector cells and by non-specific cell death. We combined and adjusted existing cell viability assays to develop a method that allows for highly reproducible, accurate, single cell analysis by high throughput FACS, in which non-specific cell death is corrected for. In this assay the number of living, calcein AM labeled cells that are green fluorescent are quantified by adding a fixed number of unlabeled calibration beads to the analysis. Using this modified FACS calcein AM retention method, we found EC50 values to be highly reproducible and considerably lower compared to EC50 values obtained by conventional assays, displaying the high sensitivity of this assay., (Copyright © 2016 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2016

11. Stable long-term cultures of self-renewing B cells and their applications.

Author

Kwakkenbos MJ, van Helden PM, Beaumont T, and Spits H

Subjects

Animals, Antibodies, Monoclonal biosynthesis, Antibody Formation immunology, Antibody-Producing Cells cytology, Antigen Presentation, Antigen-Presenting Cells immunology, Antigen-Presenting Cells metabolism, B-Lymphocytes cytology, Cell Culture Techniques, Cell Differentiation, Cell Transformation, Neoplastic genetics, Cell Transformation, Neoplastic metabolism, Cytidine Deaminase genetics, Cytidine Deaminase metabolism, Drug Discovery, Gene Expression Regulation, Germinal Center cytology, Germinal Center physiology, Humans, Immunologic Memory, Interleukins metabolism, Phenotype, Proto-Oncogene Proteins c-bcl-6 genetics, Proto-Oncogene Proteins c-bcl-6 metabolism, STAT3 Transcription Factor metabolism, STAT5 Transcription Factor metabolism, Signal Transduction, Vaccines immunology, bcl-X Protein genetics, bcl-X Protein metabolism, Antibody-Producing Cells immunology, Antibody-Producing Cells metabolism, B-Lymphocytes immunology, B-Lymphocytes metabolism, Cell Self Renewal

Abstract

Monoclonal antibodies are essential therapeutics and diagnostics in a large number of diseases. Moreover, they are essential tools in all sectors of life sciences. Although the great majority of monoclonal antibodies currently in use are of mouse origin, the use of human B cells to generate monoclonal antibodies is increasing as new techniques to tap the human B cell repertoire are rapidly emerging. Cloned lines of immortalized human B cells are ideal sources of monoclonal antibodies. In this review, we summarize our studies to the regulation of the replicative life span, differentiation, and maturation of B cells that led to the development of a platform that uses immortalization of human B cells by in vitro genetic modification for antibody development. We describe a number of human antibodies that were isolated using this platform and the application of the technique in other species. We also discuss the use of immortalized B cells as antigen-presenting cells for the discovery of tumor neoantigens., (© 2016 The Authors. Immunological Reviews Published by John Wiley & Sons Ltd.)

Published

2016

12. Genetic manipulation of B cells for the isolation of rare therapeutic antibodies from the human repertoire.

Author

Kwakkenbos MJ, Bakker AQ, van Helden PM, Wagner K, Yasuda E, Spits H, and Beaumont T

Subjects

Animals, Antibodies, Monoclonal biosynthesis, Cell Culture Techniques, Cell Separation, Cells, Cultured, DNA-Binding Proteins genetics, Drug Discovery, Genetic Engineering, Humans, Proto-Oncogene Proteins c-bcl-6, Receptors, Antigen, B-Cell genetics, Receptors, Antigen, B-Cell metabolism, bcl-X Protein genetics, Antibodies, Monoclonal isolation & purification, B-Lymphocytes physiology

Abstract

Antibody based therapies are increasingly applied to prevent and treat human disease. While the majority of antibodies currently on the market are chimeric or humanized antibodies from rodents, the focus has now shifted to the isolation and development of fully human antibodies. By retroviral transduction of B cell lymphoma-6 (BCL-6), which prevents terminal differentiation of B cells and, the anti-apoptotic gene B-cell lymphoma-extra large (Bcl-xL) into primary human B cells we efficiently immortalize antibody-producing B cells allowing the isolation of therapeutic antibodies. Selection of antigen-specific B cell clones was greatly facilitated because the transduced B cells retain surface immunoglobulin expression and secrete immunoglobulin into the culture supernatant. Surface immunoglobulin expression can be utilized to stain and isolate antigen specific B cell clones with labeled antigen. Immunoglobulins secreted in culture supernatant can directly be tested in functional assays to identify unique B cell clones. Here we describe the key features of our Bcl-6/Bcl-xL culture platform (AIMSelect)., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2014

13. CD4+ T-cell epitopes associated with antibody responses after intravenously and subcutaneously applied human FVIII in humanized hemophilic E17 HLA-DRB1*1501 mice.

Author

Steinitz KN, van Helden PM, Binder B, Wraith DC, Unterthurner S, Hermann C, Schuster M, Ahmad RU, Weiller M, Lubich C, de la Rosa M, Schwarz HP, and Reipert BM

Subjects

Animals, Antigen Presentation, CD4-Positive T-Lymphocytes metabolism, Dendritic Cells cytology, Dendritic Cells immunology, Dendritic Cells metabolism, HLA-DRB1 Chains metabolism, Haplotypes genetics, Hemophilia A metabolism, Hemophilia A pathology, Humans, Injections, Intravenous, Injections, Subcutaneous, Male, Mice, Recombinant Proteins administration & dosage, Recombinant Proteins genetics, Recombinant Proteins metabolism, Antibody Formation immunology, CD4-Positive T-Lymphocytes immunology, Disease Models, Animal, Epitopes, T-Lymphocyte immunology, Factor VIII administration & dosage, Factor VIII immunology, HLA-DRB1 Chains immunology, Hemophilia A immunology

Abstract

Today it is generally accepted that B cells require cognate interactions with CD4(+) T cells to develop high-affinity antibodies against proteins. CD4(+) T cells recognize peptides (epitopes) presented by MHC class II molecules that are expressed on antigen-presenting cells. Structural features of both the MHC class II molecule and the peptide determine the specificity of CD4(+) T cells that can bind to the MHC class II-peptide complex. We used a new humanized hemophilic mouse model to identify FVIII peptides presented by HLA-DRB1*1501. This model carries a knockout of all murine MHC class II molecules and expresses a chimeric murine-human MHC class II complex that contains the peptide-binding sites of the human HLA-DRB1*1501. When mice were treated with human FVIII, the proportion of mice that developed antibodies depended on the application route of FVIII and the activation state of the innate immune system. We identified 8 FVIII peptide regions that contained CD4(+) T-cell epitopes presented by HLA-DRB1*1501 to CD4(+) T cells during immune responses against FVIII. CD4(+) T-cell responses after intravenous and subcutaneous application of FVIII involved the same immunodominant FVIII epitopes. Interestingly, most of the 8 peptide regions contained promiscuous epitopes that bound to several different HLA-DR proteins in in vitro binding assays.

Published

2012

14. Maintenance and break of immune tolerance against human factor VIII in a new transgenic hemophilic mouse model.

Author

van Helden PM, Unterthurner S, Hermann C, Schuster M, Ahmad RU, Schiviz AN, Weiller M, Antoine G, Turecek PL, Muchitsch EM, Schwarz HP, and Reipert BM

Subjects

Animals, Antibody Formation genetics, Antibody Formation physiology, Disease Models, Animal, Factor VIII antagonists & inhibitors, Female, Hemophilia A immunology, Hemophilia A pathology, Humans, Immune Tolerance physiology, Immunologic Memory physiology, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Models, Biological, Species Specificity, Factor VIII genetics, Factor VIII immunology, Hemophilia A genetics, Immune Tolerance genetics, Immunologic Memory genetics

Abstract

Replacement of the missing factor VIII (FVIII) is the current standard of care for patients with hemophilia A. However, the short half-life of FVIII makes frequent treatment necessary. Current efforts focus on the development of longer-acting FVIII concentrates by introducing chemical and genetic modifications to the protein. Any modification of the FVIII protein, however, risks increasing its immunogenic potential to induce neutralizing antibodies (FVIII inhibitors), and this is one of the major complications in current therapy. It would be highly desirable to identify candidates with a high risk for increased immunogenicity before entering clinical development to minimize the risk of exposing patients to such altered FVIII proteins. In the present study, we describe a transgenic mouse line that expresses a human F8 cDNA. This mouse is immunologically tolerant to therapeutic doses of native human FVIII but is able to mount an antibody response when challenged with a modified FVIII protein that possesses altered immunogenic properties. In this situation, immunologic tolerance breaks down and antibodies develop that recognize both the modified and the native human FVIII. The applicability of this new model for preclinical immunogenicity assessment of new FVIII molecules and its potential use for basic research are discussed.

Published

2011

15. Domain specificity of factor VIII inhibitors during immune tolerance induction in patients with haemophilia A.

Author

van Helden PM, Kaijen PH, Mauser-Bunschoten EP, Fischer K, van den Berg HM, and Voorberg J

Subjects

Antibody Specificity, Cohort Studies, Factor VIII administration & dosage, Factor VIII genetics, Hemophilia A complications, Hemophilia A drug therapy, Humans, Mutation, Blood Coagulation Factor Inhibitors immunology, Factor VIII immunology, Hemophilia A immunology, Immune Tolerance

Abstract

Introduction: Frequent administration of high dosages factor VIII (FVIII), so-called immune tolerance induction (ITI), provides an efficient strategy to eradicate inhibitory antibodies in patients with haemophilia A. At present, our knowledge on the characteristics of inhibitory antibodies in patients undergoing ITI is limited., Aim: In this study we characterized the domain specificity of FVIII inhibitors in 11 haemophilia A patients during ITI., Results: In three of six patients who were successfully tolerized, inhibitory antibodies were directed predominantly against the FVIII light chain. In two other patients within this group, a significant contribution of A2 antibodies was observed which did not change during treatment. In the sixth patient the relative contribution of A2 inhibitors declined which coincided with an increase in antilight chain antibodies. In four of five patients who failed ITI, A2 inhibitors were observed. In two patients the contribution of A2 inhibitors increased during treatment, while in two other patients the contribution of A2 inhibitor remained constant. The fifth patient had inhibitory antibodies predominantly directed against the FVIII light chain., Conclusion: Overall, our findings revealed changes in domain specificity of FVIII antibodies in five of 11 patients analysed. Remarkably, antibodies exclusively directed towards the light chain of FVIII were predominantly observed in patients who were successfully tolerized., (© 2010 Blackwell Publishing Ltd.)

Published

2010

16. Factor VIII-specific B cell responses in haemophilia A patients with inhibitors.

Author

van Helden PM, Van Haren SD, Fijnvandraat K, van den Berg HM, and Voorberg J

Subjects

Blood Coagulation Factor Inhibitors metabolism, Enzyme-Linked Immunosorbent Assay, Factor VIII therapeutic use, Hemophilia A therapy, Humans, Risk Factors, B-Lymphocytes immunology, Factor VIII immunology, Hemophilia A immunology, Immune Tolerance, Immunologic Memory immunology

Abstract

Development of inhibitory antibodies to factor VIII (FVIII) provides a major complication of replacement therapy in patients with haemophilia A. The risk of inhibitor formation is influenced by the underlying FVIII gene defect. Moreover, genetic determinants in the promoter region of IL-10 and TNFalpha have been linked to an increased risk of inhibitor development. Recent cohort-studies have provided evidence that the risk of inhibitor formation is linked to intensity of treatment. Eradication of FVIII inhibitors can be achieved by frequent infusion of high dosages of FVIII, so-called immune tolerance induction (ITI). Until now, the mechanisms involved in downmodulation of the immune response to FVIII during ITI have not been unraveled. Studies performed in an animal model for haemophilia A have suggested that elimination of FVIII-specific memory B cells by high dosages of FVIII contributes to the decline in FVIII inhibitor levels during ITI. Limited knowledge is available with respect to the development and persistence of FVIII-specific memory B cells in patients with haemophilia A. Two recent studies suggest that the frequency of peripheral FVIII-specific memory B cells in haemophilia A patients with inhibitors range from <0.01 to 0.40% of that of total IgG(+) B cells. No or very low frequencies of FVIII-specific memory B cells are observed in haemophilia A patients without inhibitors and in patients treated successfully by ITI. Possible implications of these findings are discussed in the context of currently available information on the role of antigen-specific memory B cells and long-living antibody producing plasma cells in humoral immunity.

Published

2010

17. Opportunities and limitations of mouse models humanized for HLA class II antigens.

Author

Reipert BM, Steinitz KN, van Helden PM, Unterthurner S, Schuster M, Ahmad RU, Ilas J, and Schwarz HP

Subjects

Animals, Factor VIII immunology, Hemophilia A immunology, Humans, Mice, Mice, Transgenic, Histocompatibility Antigens Class II immunology, Immunity

Abstract

MHC class II molecules are essential for shaping the CD4+ T-cell repertoire in the thymus and for selecting antigenic peptides that are presented to CD4+ T cells in the periphery. A range of different mouse models humanized for HLA class II antigens have been developed to study the regulation of MHC-class II restricted immune responses. These mouse models have been used to identify immunodominant peptides that trigger diseases and to characterize the interactions of T-cell receptors with disease-associated peptides and MHC class II molecules. Peptides presented to CD4+ T cells in these mouse models were shown to be similar to peptides presented to CD4+ T cells in patients who carry the same MHC class II haplotype. Opportunities and limitations associated with these mouse models will be discussed and the potential application of these models for understanding the regulation of antibody responses against factor VIII in hemophilia A will be indicated.

Published

2009

18. Discordant antibody response in monozygotic twins with severe haemophilia A caused by intensive treatment.

Author

Gouw SC, ter Avest PC, van Helden PM, Voorberg J, and van den Berg HM

Subjects

Child, Preschool, Factor VIII adverse effects, Factor VIII immunology, Hemarthrosis complications, Hemarthrosis drug therapy, Hemophilia A complications, Hemophilia A drug therapy, Humans, Male, Severity of Illness Index, Twins, Monozygotic, Blood Coagulation Factor Inhibitors immunology, Factor VIII therapeutic use, Hemarthrosis immunology, Hematoma, Subdural, Intracranial diagnosis, Hemophilia A immunology

Abstract

Both genetic factors and environmental factors are suggested to play a role in the aetiology of inhibitor development in patients with severe haemophilia A. Monozygotic twins are ideal candidates to study the influence of environmental factors. We describe a pair of 3-year-old monozygotic twin brothers with severe haemophilia A. Prenatal diagnosis confirmed the presence of an intron 22 inversion. Other patient-related factors such as birth weight, vaccinations and the duration of breastfeeding were similar. At the age of 7 months, one boy suffered from a spontaneous subdural haematoma, which needed complete correction of haemostasis with continuous infusion of a third-generation recombinant factor VIII. A persistent high-titre inhibitor with severe clinical symptoms developed, that could only be eradicated with high-dose immune tolerance induction (ITI) for 36 months in combination with rituximab therapy. His twin brother first received treatment at 9 months of age with the same FVIII product. After treatment on nine exposure days, he developed a low-titre inhibitor at the age of 14.5 months. Unlike his brother, he was tolerized without difficulties with low-dose ITI within 2 months. The discordant antibody responses were underlined by dissimilar IgG1 and IgG4 levels in their plasma. The discordant immune response to FVIII in this pair of monozygotic twin brothers seemed to be related to intensity of treatment and severity of bleeds. This confirms that these environmental factors play an additional role in the development of inhibitors.

Published

2009

19. IgG subclasses of anti-FVIII antibodies during immune tolerance induction in patients with hemophilia A.

Author

van Helden PM, van den Berg HM, Gouw SC, Kaijen PH, Zuurveld MG, Mauser-Bunschoten EP, Aalberse RC, Vidarsson G, and Voorberg J

Subjects

Adolescent, Adult, Child, Child, Preschool, Enzyme-Linked Immunosorbent Assay, Factor VIII administration & dosage, Hemophilia A complications, Hemophilia A drug therapy, Humans, Infant, Factor VIII immunology, Hemophilia A immunology, Immune Tolerance, Immunoglobulin G blood

Abstract

The eradication of inhibitory antibodies in patients with haemophilia A can be accomplished by frequent administration of high or intermediate doses of factor VIII (FVIII), so-called immune tolerance induction (ITI). This study monitored the distribution of IgG subclasses of anti-FVIII antibodies during ITI. FVIII-specific antibodies of subclass IgG1 were detected in all inhibitor patients tested, anti-FVIII IgG4 in 16, IgG2 in 10 and IgG3 in one of 20 patients analysed. Levels of anti-FVIII IgG1 and IgG4 correlated well with inhibitor titres as measured by Bethesda assay. In low-titre inhibitor patients, anti-FVIII antibodies consisted primarily of subclass IgG1 whereas, anti-FVIII antibodies of subclass IgG4 were more prominent in patients with high titre inhibitors who needed prolonged treatment or who failed ITI. Longitudinal analysis of 14 patients undergoing ITI revealed that the relative contribution of IgG subclasses was constant for most of the patients analysed. In two patients, the relative contribution of IgG4 increased during ITI. Overall, our findings document the distribution and dynamics of anti-FVIII IgG subclasses during ITI. Future studies will need to address whether monitoring the relative contribution of anti-FVIII subclasses IgG1 and IgG4 may be useful for the identification of patients who are at risk of failing ITI.

Published

2008

20. Factor VIII-specific memory B cells in patients with hemophilia A.

Author

van Helden PM, Kaijen PH, Fijnvandraat K, van den Berg HM, and Voorberg J

Subjects

Antibodies blood, Enzyme-Linked Immunosorbent Assay, Humans, Immune Tolerance, Immunologic Memory, B-Lymphocytes immunology, Factor VII immunology, Hemophilia A immunology

Published

2007

21. Mechanisms of action of immune tolerance induction against factor VIII in patients with congenital haemophilia A and factor VIII inhibitors.

Author

Reipert BM, van Helden PM, Schwarz HP, and Hausl C

Subjects

Animals, Antibody Formation, Autoantibodies immunology, Autoimmune Diseases immunology, Coagulants therapeutic use, Factor VIII therapeutic use, Hemophilia A therapy, Humans, Immune Tolerance, Immunologic Memory, Models, Animal, Blood Coagulation Factor Inhibitors immunology, Factor VIII immunology, Hemophilia A immunology

Abstract

In its most severe form, haemophilia A is a life-threatening haemorrhagic bleeding disorder that is caused by mutations in the factor VIII (FVIII) gene. About 25% of patients who receive replacement therapy with intravenous FVIII products develop neutralising antibodies (FVIII inhibitors) that inhibit the function of substituted FVIII. Long-term application of high or low doses of FVIII has evolved as an effective strategy for eradicating antibodies and inducing long-lasting immune tolerance. Despite clinical experience with the therapy, little is known about the immunological mechanisms that cause the down modulation of FVIII-specific immune responses or the induction of long-lasting immune tolerance against FVIII. This review summarises current knowledge of the immunological mechanisms that might be involved in the induction of immune tolerance against FVIII in patients with haemophilia A who have FVIII inhibitors. In addition to data from patients with haemophilia A, data from patients who have had organ transplants or have immune-related disorders, such as autoimmune diseases, are considered as well as data from animal models.

Published

2007

22. Tolerance to factor VIII in a transgenic mouse expressing human factor VIII cDNA carrying an Arg(593) to Cys substitution.

Author

Bril WS, van Helden PM, Hausl C, Zuurveld MG, Ahmad RU, Hollestelle MJ, Reitsma PH, Fijnvandraat K, van Lier RA, Schwarz HP, Mertens K, Reipert BM, and Voorberg J

Subjects

Animals, Arginine, Cysteine, DNA, Complementary, Factor VIII administration & dosage, Factor VIII immunology, Humans, Mice, Mice, Knockout, Mice, Transgenic, Models, Animal, Amino Acid Substitution, Factor VIII genetics, Immune Tolerance genetics, Isoantibodies blood

Abstract

Inhibitory antibodies develop in approximately 25% of patients with severe hemophilia. A following treatment with factorVIII. In E-16KO or E-17KO mice, in which the factor VIII gene has been inactivated by insertion of a neo cassette, inhibitors develop following administration of factor VIII. Here, we describe the generation of transgenic mice expressing human factor VIII-R593C (huFVIII-R593C). Human factor VIII-R593C cDNA under control of a mouse albumin enhancer/promoter was injected into fertilized oocytes. Analysis of transgenic mice revealed that human factor VIII-R593C was expressed in the liver. Transgenic mice were crossed with factor VIII-deficient mice (E-16KO mice). In plasma of E-16KO mice antibodies were detected after five serial intravenous injections of factor VIII, while plasma of huFVIII-R593C/E-16KO mice did not contain detectable levels of antibodies. No antibody secreting cells were observed in either spleen or bone marrow of huFVIII-R593C/E-16KO mice. Also, factor VIII-specific memory B cells were not observed in the spleen of huFVIII-R593C/E-16KO mice. Analysis of T cell responses revealed that splenocytes derived of E-16KO mice secreted IL-10 and IFN-gamma following restimulation with factor VIII in vitro. In contrast, no factor VIII-specific T cell responses were observed in huFVIII-R593C/E-16KO mice. These results indicate that huFVIII-R593C/E-16KO mice are tolerant to intravenously administered factor VIII. It is anticipated that this model may prove useful for studying immune responses in the context of factor VIII gene therapy.

Published

2006