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1. Polymyositis in Kooiker dogs is associated with a 39 kb deletion upstream the IL21/IL2 genes

Author

Leegwater, Peter, Opmeer, Yvet, van Steenbeek, Frank, Rozendom, Claudia, van Kooten, Peter, Rutten, VP, Fieten, Hille, Hytönen, Marjo K, Lohi, Hannes, Mandigers, Paul, Leegwater, Peter, Opmeer, Yvet, van Steenbeek, Frank, Rozendom, Claudia, van Kooten, Peter, Rutten, VP, Fieten, Hille, Hytönen, Marjo K, Lohi, Hannes, and Mandigers, Paul

Abstract

An inflammatory myopathy with characteristics of polymyositis is prevalent in the ‘Nederlandse Kooikerhondje’ dog breed. A genome wide association study of 33 cases and 106 controls indicated the involvement of a region on chromosome 19 containing the cytokine gene pair IL21 and IL2 (praw = 2.1*10-14). Next generation DNA sequencing revealed that 8 cases shared a 39 kb deletion, situated 10 kb upstream of IL21. Of the 102 cases with available DNA, 66 were homozygous, 34 were heterozygous and only 2 cases were clear of the deletion. The frequency of the deletion allele in a random sample of the Kooiker dog breed was 0.25. Postulating causality, the penetrance of the disease phenotype was estimated at 5-15% for homozygous dogs and 0.5-2% for dogs that are heterozygous for the deletion. Leukocytes of affected, untreated dogs that were homozygous for the deletion overexpress IL21 and IL2 after stimulation with mitogens. We suggest that elements located 10 – 49 kb upstream of the IL21/IL2 gene pair play an important role in the regulation of the canine genes and that deletion of these elements is a risk factor for inflammatory myopathy in Kooiker dogs. Our results imply that distant variants upstream of IL21 could also be important for human autoimmune diseases that were found to be associated with the IL21/IL2 chromosome region.

Published
2024

11. Leucinostatin acts as a co-inducer for heat shock protein 70 in cultured canine retinal pigment epithelial cells

Author

LS Immunologie, dI&I RA-I&I I&I, Immunologie, CS_Welfare & emerging diseases, Lyu, Qingkang, Ludwig, Irene S, Kooten, Peter J S, Sijts, Alice J A M, Rutten, Victor P M G, van Eden, Willem, Broere, Femke, LS Immunologie, dI&I RA-I&I I&I, Immunologie, CS_Welfare & emerging diseases, Lyu, Qingkang, Ludwig, Irene S, Kooten, Peter J S, Sijts, Alice J A M, Rutten, Victor P M G, van Eden, Willem, and Broere, Femke

Published
2020

15. Additional file 1: of Evidence of high EEHV antibody seroprevalence and spatial variation among captive Asian elephants (Elephas maximus) in Thailand

Author

Taweepoke Angkawanish, Nielen, Mirjam, Vernooij, Hans, Brown, Janine, Kooten, Peter, Doel, Petra, Schaftenaar, Willem, Kannika Na Lampang, and Rutten, Victor

Abstract

Figure S1. Stacked bar plots with numbers of negative and positive animals per herd (ranked on herd size). Using as definitions for a positive sample: both OD ratio ≥ 3 (graph a) and OD ratio ≥ 4 (graph b). (PDF 58 kb)

Published
2019
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16. Additional file 2: of Evidence of high EEHV antibody seroprevalence and spatial variation among captive Asian elephants (Elephas maximus) in Thailand

Author

Taweepoke Angkawanish, Nielen, Mirjam, Vernooij, Hans, Brown, Janine, Kooten, Peter, Doel, Petra, Schaftenaar, Willem, Kannika Na Lampang, and Rutten, Victor

Abstract

Table S1. Seroprevalence based on an EEHV1A glycoprotein B protein antigen specific ELISA of elephants sampled throughout Thailand (nâ =â 994) between 2010 and 2015, and the percentage of samples testing positive1, inconclusive2 or negative3 relative to potential EEHV risk factors based on different interpretation modalities: 1:100 dilution; 1:200 dilution. (PDF 58 kb)

Published
2019
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17. Additional file 3: of Evidence of high EEHV antibody seroprevalence and spatial variation among captive Asian elephants (Elephas maximus) in Thailand

Author

Taweepoke Angkawanish, Nielen, Mirjam, Vernooij, Hans, Brown, Janine, Kooten, Peter, Doel, Petra, Schaftenaar, Willem, Kannika Na Lampang, and Rutten, Victor

Abstract

Table S2. Univariable regression analysis of potential risk factors for the presence of EEHV antibodies in elephants sampled throughout Thailand between 2010 and 2015 (n = 994) based on an EEHV1A glycoprotein B protein antigen specific ELISA. Seroprevalence is based on strict cutoff: positive if both OD ratio’s > 4. (PDF 52 kb)

Published
2019
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19. Peptide-induced nasal tolerance for a mycobacterial heat shock protein 60 T cell epitope in rats suppresses both adjuvant arthritis and nonmicrobially induced experimental arthritis

Author

Prakken, Berent J., Zee, Ruurd van der, Anderton, Stephen M., Kooten, Peter J.S. van, Kuis, Wietse, and Eden, Willem van

Subjects
Rheumatoid arthritis -- Physiological aspects, Heat shock proteins -- Physiological aspects, T cells -- Physiological aspects, Rats -- Physiological aspects, Science and technology
Abstract

Adjuvant arthritis (AA) can be induced in Lewis rats by immunization with mycobacterial antigens. Passive transfer of a T cell clone recognizing the 180-188 amino acid sequence in mycobacterial heat shock protein 60 (hsp60) was found to induce AA. In the present study, we investigated whether tolerance was obtained for this AA-associated T cell epitope after intranasal or s.c. administration of a peptide containing this epitope. Two 15-mer peptides containing the mycobacterial hsp60 sequences 176-190 and 211-225 were used; 176-190 contained the T cell epitope 180-188, which was recognized by the arthritogenic T cell clone A2b and was the immunodominant hsp60 T cell epitope after induction of AA, and 211-225 contained a T cell epitope that was recognized both after induction of arthritis with whole Mycobacterium tuberculosis and after immunization with mycobacterial hsp60. In rats treated intranasally or subcutaneously with 176-190 and immunized with mycobacterial hsp60, proliferative responses to 176-190 were reduced. Proliferative responses to 211-225 and to whole mycobacterial hsp60 were not affected. AA was inhibited intranasally in the 176-190-treated rats but not in the 211-225-treated rats. Moreover, intranasal 176-190 led to similar arthritis-protective effects in a nonmicrobially induced experimental arthritis (avridine-induced arthritis). Therefore, tolerance for a disease-triggering, microbial cartilage-mimicking epitope may cause resistance to arthritis irrespective of the actual trigger leading to development of the disease.

Published
1997

20. Evidence of high EEHV antibody seroprevalence and spatial variation among captive Asian elephants (Elephas maximus) in Thailand

Author

dFAH AVR, LS Evidence Based Vet Medicine, LS Theoretische Epidemiologie, dI&I RA-I&I I&I, LS Immunologie, Immunologie, Angkawanish, Taweepoke, Nielen, Mirjam, Vernooij, Hans, Brown, Janine L, van Kooten, Peter J S, van den Doel, Petra B, Schaftenaar, Willem, Na Lampang, Kannika, Rutten, Victor P M G, dFAH AVR, LS Evidence Based Vet Medicine, LS Theoretische Epidemiologie, dI&I RA-I&I I&I, LS Immunologie, Immunologie, Angkawanish, Taweepoke, Nielen, Mirjam, Vernooij, Hans, Brown, Janine L, van Kooten, Peter J S, van den Doel, Petra B, Schaftenaar, Willem, Na Lampang, Kannika, and Rutten, Victor P M G

Published
2019

22. The Enigma of Heat Shock Proteins in Immune Tolerance

Author

van Eden, Willem, Jansen, Manon A A, Ludwig, Irene, van Kooten, Peter, van der Zee, Ruurd, Broere, Femke, dI&I RA-I&I I&I, and dI&I RA-I&I I&I

Subjects
lcsh:Immunologic diseases. Allergy, 0301 basic medicine, rheumatoid, Mini Review, Immunology, Arthritis, Disease, Biology, regulatory T cells, Immune tolerance, 03 medical and health sciences, 0302 clinical medicine, Immune system, cell stress, Downregulation and upregulation, Heat shock protein, medicine, Immunology and Allergy, medicine.disease, Hsp70, 030104 developmental biology, tolerance mechanisms, arthritis, 030220 oncology & carcinogenesis, heat shock proteins, HSP60, lcsh:RC581-607
Abstract

The fundamental problem of autoimmune diseases is the failure of the immune system to downregulate its own potentially dangerous cells, which leads to destruction of tissue expressing the relevant autoantigens. Current immunosuppressive therapies offer relief but fail to restore the basic condition of self-tolerance. They do not induce long-term physiological regulation resulting in medication-free disease remissions. Heat shock proteins (HSPs) have shown to possess the capacity of inducing lasting protective immune responses in models of experimental autoimmune diseases. Especially mycobacterial HSP60 and HSP70 were shown to induce disease inhibitory IL-10-producing regulatory T cells in many different models. This in itself may seem enigmatic, since based on earlier studies, HSPs were also coined sometimes as pro-inflammatory damage-associated molecular patterns. First clinical trials with HSPs in rheumatoid arthritis and type I diabetes have also indicated their potential to restore tolerance in autoimmune diseases. Data obtained from the models have suggested three aspects of HSP as being critical for this tolerance promoting potential: 1. evolutionary conservation, 2. most frequent cytosolic/nuclear MHC class II natural ligand source, and 3. upregulation under (inflammatory) stress. The combination of these three aspects, which are each relatively unique for HSP, may provide an explanation for the enigmatic immune tolerance promoting potential of HSP.

Published
2017

23. Dynamics of APC recruitment at the site of injection following injection of vaccine adjuvants

Author

van Aalst, Susan, Ludwig, Irene Stephanie, van Kooten, Peter Johannes Sylvester, van der Zee, Ruurd, van Eden, Willem, Broere, Femke, LS Immunologie, dI&I RA-I&I I&I, LS Immunologie, and dI&I RA-I&I I&I

Subjects
0301 basic medicine, medicine.medical_treatment, T cell, Antigen presentation, MF59, Antigen-Presenting Cells, Mechanism of action, Injections, Intramuscular, Vaccine adjuvant, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, Adjuvants, Immunologic, Medicine, Animals, Site of injection, Innate immunity, Mice, Inbred BALB C, Innate immune system, General Veterinary, General Immunology and Microbiology, business.industry, Muscles, Public Health, Environmental and Occupational Health, Immunity, Innate, APC, 030104 developmental biology, Infectious Diseases, Cytokine, medicine.anatomical_structure, Immunology, Muscle immunity, Molecular Medicine, Female, business, Adjuvant, 030215 immunology
Abstract

Vaccines often contain adjuvants to strengthen the response to the vaccine antigen. However, their modes of action at the site of injection (SOI) are poorly understood. Therefore, we assessed the local effects of adjuvant on the innate immune system in mice. We investigated the safe, widely used adjuvants MF59 and aluminum hydroxide (alum), as well as trehalose-6,6???-dibehenate (TDB), Complete Freund's Adjuvant (CFA) and the Toll-Like-Receptor-ligands lipopolysaccharide (LPS) and Pam3CysSerLys4 (Pam3CSK4). We assessed muscle immune cell infiltration after adjuvant injection and observed 16??h post immunization (hpi) an increased influx with CFA, MF59 and TDB, but not with alum, LPS or Pam3CSK4. An elevated influx with the latter three became visible only 72??hpi. Contribution of granulocytes, macrophages and dendritic cells to the influx differed per adjuvant and in time. Adjuvants generally induced a local pro-inflammatory micro-milieu that was transient except for CFA and TDB. The gene expression of CXCL-1, CCL-2 and CCL-5, involved in recruitment of immune cells, varied per adjuvant and corresponded grossly with the observed influx of granulocytes and monocytes/macrophages. Muscles injected with CFA or MF59 (when co-injected with peptide) resulted in APC ex vivo capable to induce proliferation of peptide-specific T-cells. By adding in vitro an excess of peptide to the APC/T cell co-cultures, we observed an adjuvant-enhanced co-stimulation or antigen presentation by APC after CFA- but not MF59-injection. After TDB-injection this effect was observed only at 72??hpi, but not 24??hpi. Thus the cellular influx profile and the local cytokine and chemokine micro-milieu in the muscle were strongly influenced by the type of adjuvant. Additionally, the capacity of muscle APC to load and present antigen was affected by the adjuvant. These findings may assist the development of novel adjuvanted vaccines in a more rational manner.

Published
2017

24. Nanoporous Microneedle Arrays Effectively Induce Antibody Responses against Diphtheria and Tetanus Toxoid

Author

de Groot, Anne Marit, Platteel, Anouk C M, Kuijt, Nico, van Kooten, Peter J S, Vos, Pieter Jan, Sijts, Alice J A M, van der Maaden, Koen, dI&I RA-I&I I&I, and dI&I RA-I&I I&I

Subjects
0301 basic medicine, lcsh:Immunologic diseases. Allergy, intradermal vaccination, Immunology, 02 engineering and technology, antigen release, tetanus, 03 medical and health sciences, nanoporous microneedles, Dermis, In vivo, Stratum corneum, medicine, Immunology and Allergy, diphtheria, Original Research, Diphtheria toxin, integumentary system, Chemistry, Diphtheria, Toxoid, 021001 nanoscience & nanotechnology, medicine.disease, humoral immune response, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Drug delivery, 0210 nano-technology, lcsh:RC581-607, Ex vivo, Biomedical engineering
Abstract

The skin is immunologically very potent because of the high number of antigen-presenting cells in the dermis and epidermis, and is therefore considered to be very suitable for vaccination. However, the skin's physical barrier, the stratum corneum, prevents foreign substances, including vaccines, from entering the skin. Microneedles, which are needle-like structures with dimensions in the micrometer range, form a relatively new approach to circumvent the stratum corneum, allowing for minimally invasive and pain-free vaccination. In this study, we tested ceramic nanoporous microneedle arrays (npMNAs), representing a novel microneedle-based drug delivery technology, for their ability to deliver the subunit vaccines diphtheria toxoid (DT) and tetanus toxoid (TT) intradermally. First, the piercing ability of the ceramic (alumina) npMNAs, which contained over 100 microneedles per array, a length of 475 µm, and an average pore size of 80 nm, was evaluated in mouse skin. Then, the hydrodynamic diameters of DT and TT and the loading of DT, TT, and imiquimod into, and subsequent release from the npMNAs were assessed in vitro. It was shown that DT and TT were successfully loaded into the tips of the ceramic nanoporous microneedles, and by using near-infrared fluorescently labeled antigens, we found that DT and TT were released following piercing of the antigen-loaded npMNAs into ex vivo murine skin. Finally, the application of DT- and TT-loaded npMNAs onto mouse skin in vivo led to the induction of antigen-specific antibodies, with titers similar to those obtained upon subcutaneous immunization with a similar dose. In conclusion, we show for the first time, the potential of npMNAs for intradermal (ID) immunization with subunit vaccines, which opens possibilities for future ID vaccination designs.

Published
2017
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25. Identification of a novel kisspeptin with high gonadotrophin stimulatory activity in the dog

Author

Albers-Wolthers, Karin H J, de Gier, Jeffrey, Kooistra, Hans S, Rutten, Victor P M G, van Kooten, Peter J S, de Graaf, Janneke J, Leegwater, Peter A J, Millar, Robert P, Schaefers-Okkens, Auke C, CSCA AVM, Advances in Veterinary Medicine, I&I RATIA-SIB, Sub Voortplanting, Sub Endocrinologie, LS Immunologie, Onderzoek, Tissue Repair, CSCA TR1, CSCA AVM, Advances in Veterinary Medicine, I&I RATIA-SIB, Sub Voortplanting, Sub Endocrinologie, LS Immunologie, Onderzoek, Tissue Repair, and CSCA TR1

Subjects
Luteinizing hormone, Endocrinology, Diabetes and Metabolism, kiss1, Beagle, Receptors, G-Protein-Coupled, Canine, Gonadotropin-Releasing Hormone, Follicle-stimulating hormone, 0302 clinical medicine, Endocrinology, Kisspeptin, Reproduction, Receptor, Kisspeptins, 0303 health sciences, 030219 obstetrics & reproductive medicine, Estradiol, Chemistry, Biological activity, 3. Good health, Dose–response relationship, Area Under Curve, hormones, hormone substitutes, and hormone antagonists, medicine.medical_specialty, endocrine system, kiss1r, GPR54, 03 medical and health sciences, Cellular and Molecular Neuroscience, Dogs, Internal medicine, medicine, Animals, Humans, RNA, Messenger, 030304 developmental biology, Analysis of Variance, Dose-Response Relationship, Drug, Endocrine and Autonomic Systems, Bitch, Luteinizing Hormone, Gene Expression Regulation, Follicle Stimulating Hormone, Receptors, Kisspeptin-1, Hormone
Abstract

Kisspeptin (KISS1) and its receptor (KISS1r) are essential for normal reproductive function in many species, but the role of kiss1/kiss1r signalling in the dog has not yet been elucidated. The aims of this study were to identify the canine kiss1 and kiss1r genes and to determine gonadotrophin and oestradiol stimulatory activity of KP-10, the shortest biologically active form of KISS1. Canine kiss1 and kiss1r genes were localized by comparing the reference dog genome with relevant human cDNA sequences, using BLASTn software. The amino acid sequence of canine KP-10 (YNWNVFGLRY) differs at two positions from human KP-10 (YNWNSFGLRF). A single bolus of canine KP-10 was administered intravenously to anoestrous Beagle bitches in dosages of 0, 0.1, 0.2, 0.3, 0.5, 1, 5, 10, and 30 μg/kg. Blood samples were collected before and after canine KP-10 administration for the measurement of plasma luteinizing hormone (LH, all doses), follicle-stimulating hormone (FSH) and oestradiol (1-30 μg/kg). From 0.2 μg/kg onwards, canine KP-10 resulted in a rapid and robust rise in plasma LH concentration (max. at 10 min). KP-10 also resulted in a rapid and robust rise in plasma FSH concentration (max. at 10-20 min). Plasma oestradiol concentration increased significantly after dosages of 1, 5, and 10 μg/kg and reached a maximum at 60-90 min. In conclusion, canine KP-10 is a potent kisspeptin which elicits robust gonadotrophin and oestradiol responses in anoestrous bitches, suggesting that canine kiss1/kiss1r are cogent targets for modulating reproduction in dogs.

Published
2014

27. The Enigma of Heat Shock Proteins in Immune Tolerance

Author

dI&I RA-I&I I&I, van Eden, Willem, Jansen, Manon A A, Ludwig, Irene, van Kooten, Peter, van der Zee, Ruurd, Broere, Femke, dI&I RA-I&I I&I, van Eden, Willem, Jansen, Manon A A, Ludwig, Irene, van Kooten, Peter, van der Zee, Ruurd, and Broere, Femke

Published
2017

29. Generation of the First TCR Transgenic Mouse with CD4+ T Cells Recognizing an Anti-inflammatory Regulatory T Cell-Inducing Hsp70 Peptide

Author

Jansen, Manon A A, Van Herwijnen, Martijn J C, Van Kooten, Peter J S, Hoek, Aad, Van Der Zee, Ruurd, Van Eden, Willem, Broere, Femke, LS Immunologie, LS Celbiologie-Algemeen, dI&I RA-I&I I&I, LS Immunologie, LS Celbiologie-Algemeen, and dI&I RA-I&I I&I

Subjects
lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Regulatory T cell, T cell, Immunology, Autoimmunity, chemical and pharmacologic phenomena, Streptamer, Biology, Epitope, hybridoma, regulatory T cells, 03 medical and health sciences, Interleukin 21, 0302 clinical medicine, Transgenic mouse, medicine, Immunology and Allergy, Cytotoxic T cell, Heat shock protein 70, heat shock protein 70, IL-2 receptor, Original Research, T-cell receptor, autoimmunity, hemic and immune systems, Regulatory T cells, Cell biology, transgenic mouse, 030104 developmental biology, medicine.anatomical_structure, lcsh:RC581-607, Hybridoma, 030215 immunology
Abstract

Antigen-specific regulatory T cells (Tregs) directed at self-antigens are difficult to study since suitable specific tools to isolate and characterize these cells are lacking. A T cell receptor (TCR)-transgenic mouse would generate possibilities to study such antigen-specific T cells. As was shown previously, immunization with the mycobacterial heat shock protein 70 derived peptide B29 and its mouse homologues mB29a and mB29b induced anti-inflammatory responses. Furthermore, B29 induced antigen-specific regulatory T cells (Tregs) in vivo. To study mB29b specific Tregs, we isolated the TCR from T cell hybridomas generated against mB29b and produced a TCR transgenic mouse that expresses a MHC-class II restricted mB29b-specific TCR. These TCR transgenic CD4+ T cells were found to cross react with the B29 epitope as identified with peptide induced proliferation and IL-2 production. Thus, we have successfully generated a novel mouse model with antigen-specific CD4+ T cells that recognize self and bacterial heat shock protein (Hsp) 70 derived peptides. With this novel mouse model, it will be possible to study primary antigen specific T cells with specificity for a regulatory HSP70 T cell epitope. This will enable the isolation and characterization CD4+CD25+ Tregs with a proven specificity. This will provide useful knowledge of the induction, activation and mode of action of Hsp70- specific Tregs, for instance during experimental arthritis.

Published
2016

30. Pathogenicity of Bovine Neonatal Pancytopenia-associated vaccine-induced alloantibodies correlates with Major Histocompatibility Complex class I expression

Author

Benedictus, Lindert, Luteijn, Rutger D, Otten, Henny, Jan Lebbink, Robert, van Kooten, Peter J S, Wiertz, Emmanuel J H J, Rutten, Victor P M G, Koets, Ad P, Infection & Immunity, dIRAS RA-I&I RA, Risk Assessment, LS Immunologie, Sub Immunologie, Infection & Immunity, dIRAS RA-I&I RA, Risk Assessment, LS Immunologie, and Sub Immunologie

Subjects
Pancytopenia, Cattle Diseases, Research Support, Major histocompatibility complex, Article, Cell Line, Antigen, Antibody Specificity, Isoantibodies, Pregnancy, MHC class I, Journal Article, medicine, Animals, Humans, cardiovascular diseases, Non-U.S. Gov't, Multidisciplinary, Bovine Neonatal Pancytopenia, biology, Adverse effects, Integrin beta1, Research Support, Non-U.S. Gov't, Histocompatibility Antigens Class I, Viral Vaccines, medicine.disease, alloantibodies, Virology, Histocompatibility, medicine.anatomical_structure, Immunology, biology.protein, cardiovascular system, very late antigen-3, Cattle, Female, Bone marrow, Antibody, Lymphocytopenia, human activities, hormones, hormone substitutes, and hormone antagonists
Abstract

Bovine Neonatal Pancytopenia (BNP), a fatal bleeding syndrome of neonatal calves, is caused by maternal alloantibodies absorbed from colostrum and is characterized by lymphocytopenia, thrombocytopenia and bone marrow hypoplasia. An inactivated viral vaccine is the likely source of alloantigens inducing BNP-associated alloantibodies in the dam. In this study the specificity of BNP alloantibodies was assessed and was linked to the pathology of BNP. We demonstrated that Major Histocompatibility Complex class I (MHC I) and Very Late Antigen-3, an integrin α3/β1 heterodimer, were the major targets of BNP alloantibodies. However, alloantibody binding to various bovine cell types correlated with MHC I expression, rather than integrin β1 or α3 expression. Likewise, alloantibody-dependent complement-mediated cell lysis correlated strongly with MHC I expression. Examination of several tissues of third trimester bovine foetuses revealed that cells, shown to be affected in calves with BNP, were characterized by high MHC class I expression and high levels of alloantibody binding. We conclude that in spite of the heterogeneous specificity of BNP associated maternal alloantibodies, MHC I-specific antibodies mediate the pathogenicity of BNP in the calf and that cells with high MHC I expression were preferentially affected in BNP.

Published
2015

31. Identification of an Activating Chicken Ig-like Receptor Recognizing Avian Influenza Viruses

Author

Jansen, Christine A, van Haarlem, Daphne A, Sperling, Beatrice, van Kooten, Peter J, de Vries, Erik, Viertlboeck, Birgit C, Vervelde, Lonneke, Göbel, Thomas W, Jansen, Christine A, van Haarlem, Daphne A, Sperling, Beatrice, van Kooten, Peter J, de Vries, Erik, Viertlboeck, Birgit C, Vervelde, Lonneke, and Göbel, Thomas W

Abstract

Chicken Ig-like receptors (CHIRs) represent a multigene family encoded by the leukocyte receptor complex that encodes a variety of receptors that are subdivided into activating CHIR-A, inhibitory CHIR-B, and bifunctional CHIR-AB. Apart from CHIR-AB, which functions as an Fc receptor, CHIR ligands are unknown. In the current study, we used a panel of different BWZ.36 CHIR reporter cells to identify an interaction between specific CHIRs and avian influenza virus (AIV). The specificity of the CHIR-AIV interaction was further demonstrated using CHIR fusion proteins that bound to AIV-coated plates and were able to reduce the interaction of reporter cells with AIV. There was no difference in binding of CHIR to different AIV strains. Furthermore, CHIR fusion proteins reduced AIV-induced in vitro activation of NK cells obtained from lungs of AIV-infected animals, as judged by the lower frequency of CD107(+) cells. Because the original CHIR reporter lines were generated based on sequence information about extracellular CHIR domains, we next identified a full-length CHIR that displayed similar binding to AIV. The sequence analysis identified this CHIR as a CHIR-A. Neuraminidase treatment of coated CHIR-human Ig proteins reduced binding of trimeric H5 proteins to CHIR. This suggests that the interaction is dependent on sialic acid moieties on the receptor. In conclusion, this article identifies AIV as a ligand of CHIR-A and describes the functional consequences of this interaction.

Published
2016

32. Generation of the first TCR transgenic mouse with CD4+ T cells recognizing an anti-inflammatory regulatory T cell-inducing Hsp70 peptide

Author

LS Immunologie, LS Celbiologie-Algemeen, dI&I RA-I&I I&I, Jansen, Manon A A, Van Herwijnen, Martijn J C, Van Kooten, Peter J S, Hoek, Aad, Van Der Zee, Ruurd, Van Eden, Willem, Broere, Femke, LS Immunologie, LS Celbiologie-Algemeen, dI&I RA-I&I I&I, Jansen, Manon A A, Van Herwijnen, Martijn J C, Van Kooten, Peter J S, Hoek, Aad, Van Der Zee, Ruurd, Van Eden, Willem, and Broere, Femke

Published
2016

33. Identification of an Activating Chicken Ig-like Receptor Recognizing Avian Influenza Viruses

Author

LS Immunologie, LS Virologie, dIRAS RA-I&I RA, Jansen, Christine A, van Haarlem, Daphne A, Sperling, Beatrice, van Kooten, Peter J, de Vries, Erik, Viertlboeck, Birgit C, Vervelde, Lonneke, Göbel, Thomas W, LS Immunologie, LS Virologie, dIRAS RA-I&I RA, Jansen, Christine A, van Haarlem, Daphne A, Sperling, Beatrice, van Kooten, Peter J, de Vries, Erik, Viertlboeck, Birgit C, Vervelde, Lonneke, and Göbel, Thomas W

Published
2016

34. APL1, an altered peptide ligand derived from human heat-shock protein 60, increases the frequency of Tregs and its suppressive capacity against antigen responding effector CD4 + T cells from rheumatoid arthritis patients

Author

LS Immunologie, Barberá, Ariana, Lorenzo, Noraylis, van Kooten, Peter, van Roon, Joel, de Jager, Wilco, Prada, Dinorah, Gómez, Jorge, Padrón, Gabriel, van Eden, Willem, Broere, Femke, Del Carmen Domínguez, María, LS Immunologie, Barberá, Ariana, Lorenzo, Noraylis, van Kooten, Peter, van Roon, Joel, de Jager, Wilco, Prada, Dinorah, Gómez, Jorge, Padrón, Gabriel, van Eden, Willem, Broere, Femke, and Del Carmen Domínguez, María

Published
2016

35. Membrane-bound metallothionein 1 of murine dendritic cells promotes the expansion of regulatory T cells in vitro

Author

Spiering, Rachel, Wagenaar-Hilbers, Josée, Huijgen, Veerle, Van der Zee, Ruurd, Van Kooten, Peter J S, Van Eden, Willem, Broere, Femke, LS Immunologie, I&I RATIA-SIB, Strategic Infection Biology, LS Immunologie, I&I RATIA-SIB, and Strategic Infection Biology

Subjects
musculoskeletal diseases, Immune regulation, Cell, Mice, Transgenic, chemical and pharmacologic phenomena, macromolecular substances, Biology, Toxicology, T-Lymphocytes, Regulatory, Dendritic cells, Dexamethasone, Cell membrane, Mice, Immune system, Chlorides, stomatognathic system, medicine, Immune Tolerance, Metallothionein, Animals, RNA, Messenger, Cells, Cultured, Mice, Inbred BALB C, Stress protein, Cell Membrane, Forkhead Transcription Factors, T lymphocyte, Metallothionein 1, Phenotype, In vitro, Cell biology, Protein Transport, medicine.anatomical_structure, Zinc Compounds, embryonic structures, Female, Function (biology), Immunosuppressive Agents
Abstract

Exposure to environmental toxicants can alter a range of cellular functions involved in the immune response. Increased expression of the stress protein metallothionein 1 (MT1) is one example hereof. Previously, it has been reported that MT1 has several immunosuppressive properties. Furthermore, we earlier showed that functionally tolerogenic dendritic cells (DCs) expressed increased mRNA levels of MT1. Here, we demonstrate that dexamethasone-treated murine DCs are functionally tolerogenic and produce MT1. However, these DCs do not actively transport MT1 to the cell membrane and their regulatory function does not depend on MT1. Alternatively, ZnCl2-treated murine DCs transport MT1 to the cell surface are tolerogenic and promote the expansion of T cells with a regulatory phenotype. Moreover, the membrane-bound MT1 was shown to be essential for ZnCl2-treated DCs to exert their regulatory function. On the basis of this, MT1 can be used as a new marker for functionally tolerogenic DCs. Additionally, we have found a new mechanism for tolerogenic DCs to exert their immune regulatory function.© The Author 2013.Published by Oxford University Press on behalf of the Society of Toxicology.All rights reserved.

Published
2014

36. Hypothalamic vasotocin and tyrosine hydroxylase levels following maternal care and selection for low mortality in laying hens

Author

Hewlett, Susie E, Zeinstra, Elly C, van Eerdenburg, Frank J C M, Rodenburg, Tb, van Kooten, Peter J S, van der Staay, Franz Josef, Nordquist, Rebecca E, Emotion and Cognition, FAH E&C, Sub Emotion & Cognition, LS GZ Landbouwhuisdieren, LS Immunologie, FAH AVM, Advances in Veterinary Medicine, Emotion and Cognition, FAH E&C, Sub Emotion & Cognition, LS GZ Landbouwhuisdieren, LS Immunologie, FAH AVM, and Advances in Veterinary Medicine

Subjects
Vasopressin, Dopamine, Vasotocin, Breeding, hpa axis, Open field, chemistry.chemical_compound, Behavioral Ecology, stress, Animal Husbandry, Maternal Behavior, feather pecking behavior, Feather pecking, Behavior, Animal, Dopaminergic, General Medicine, Poultry farming, dopamine neurons, Gedragsecologie, Hypothalamus, Female, Research Article, medicine.medical_specialty, animal structures, Tyrosine 3-Monooxygenase, brain, chicken, Welfare, Biology, system, Internal medicine, medicine, Animals, Selection, Genetic, Laying hen, General Veterinary, Tyrosine hydroxylase, business.industry, social-behavior, area, veterinary(all), Endocrinology, chemistry, WIAS, business, gallus-domesticus, Chickens
Abstract

BACKGROUND: Feather pecking and cannibalism are major concerns in poultry farming, both in terms of animal welfare and farm economics. Genetic selection and introduction of (aspects of) maternal care have been suggested as potential interventions to reduce feather pecking in laying hens. Altered brain development has been proposed to reflect welfare states in animals, and can provide more insight into the underlying processes involved in feather pecking. Both vasotocin (the avian homologue of vasopressin) and dopaminergic neural circuitry have roles in control of social behaviors as well as in the stress response, and may be linked to feather pecking. Thus, the hypothalamus of adult laying hens selected for low early mortality (LML), which show low feather pecking, was examined and compared with a control line of adult laying hens selected for production characteristics only (CL). The effect of foster hen rearing on the two genetic lines and their hypothalamic morphology was also investigated. RESULTS: We demonstrated an increase in the number of neurons positive for the rate-limiting enzyme in dopamine production, tyrosine hydroxylase, in the periventricular area of the hypothalamus in the LML hens compared to CL hens. Hen-reared chicks showed more vasotocin -positive neurons in the medial pre-optic area compared to the hens raised without a hen. No correlations were found between behavior in an open field at 5-6 weeks of age, and the histology of the same hens at adulthood. CONCLUSION: The hypothalamic dopaminergic and vasotinergic systems are altered in hens following genetic selection or maternal care, indicating a potential role for these systems in feather pecking. Keywords: Hypothalamus, Vasotocin, Vasopressin, Tyrosine hydroxylase, Dopamine, Welfare, Laying hen

Published
2014

37. Pathogenicity of Bovine Neonatal Pancytopenia-associated vaccine-induced alloantibodies correlates with Major Histocompatibility Complex class I expression

Author

Infection & Immunity, dIRAS RA-I&I RA, Risk Assessment, LS Immunologie, Sub Immunologie, Benedictus, Lindert, Luteijn, Rutger D, Otten, Henny, Jan Lebbink, Robert, van Kooten, Peter J S, Wiertz, Emmanuel J H J, Rutten, Victor P M G, Koets, Ad P, Infection & Immunity, dIRAS RA-I&I RA, Risk Assessment, LS Immunologie, Sub Immunologie, Benedictus, Lindert, Luteijn, Rutger D, Otten, Henny, Jan Lebbink, Robert, van Kooten, Peter J S, Wiertz, Emmanuel J H J, Rutten, Victor P M G, and Koets, Ad P

Published
2015

38. Pathogenicity of Bovine Neonatal Pancytopenia-associated vaccine-induced alloantibodies correlates with Major Histocompatibility Complex class I expression

Author

MMB Research line 3a, Infection & Immunity, Benedictus, Lindert, Luteijn, Rutger D, Otten, Henny, Lebbink, Robert Jan, van Kooten, Peter J S, Wiertz, EJHJ, Rutten, Victor P M G, Koets, Ad P, MMB Research line 3a, Infection & Immunity, Benedictus, Lindert, Luteijn, Rutger D, Otten, Henny, Lebbink, Robert Jan, van Kooten, Peter J S, Wiertz, EJHJ, Rutten, Victor P M G, and Koets, Ad P

Published
2015

40. The immunostimulatory effect of CpG oligodeoxynucleotides on peripheral blood mononuclear cells of healthy dogs and dogs with atopic dermatitis

Author

Sub Dermatologie, LS Immunologie, Risk Assessment of Toxic and Immunomodulatory Agents, I&I RATIA-SIB, Jassies-van der Lee, Annette, Rutten, Victor, Spiering, Rachel, van Kooten, Peter, Willemse, Ton, Broere, Femke, Sub Dermatologie, LS Immunologie, Risk Assessment of Toxic and Immunomodulatory Agents, I&I RATIA-SIB, Jassies-van der Lee, Annette, Rutten, Victor, Spiering, Rachel, van Kooten, Peter, Willemse, Ton, and Broere, Femke

Published
2014

41. Hypothalamic vasotocin and tyrosine hydroxylase levels following maternal care and selection for low mortality in laying hens

Author

Emotion and Cognition, FAH E&C, Sub Emotion & Cognition, LS GZ Landbouwhuisdieren, LS Immunologie, FAH AVM, Advances in Veterinary Medicine, Hewlett, Susie E, Zeinstra, Elly C, van Eerdenburg, Frank J C M, Rodenburg, Tb, van Kooten, Peter J S, van der Staay, Franz Josef, Nordquist, Rebecca E, Emotion and Cognition, FAH E&C, Sub Emotion & Cognition, LS GZ Landbouwhuisdieren, LS Immunologie, FAH AVM, Advances in Veterinary Medicine, Hewlett, Susie E, Zeinstra, Elly C, van Eerdenburg, Frank J C M, Rodenburg, Tb, van Kooten, Peter J S, van der Staay, Franz Josef, and Nordquist, Rebecca E

Published
2014

42. Membrane-bound metallothionein 1 of murine dendritic cells promotes the expansion of regulatory T cells in vitro

Author

LS Immunologie, I&I RATIA-SIB, Strategic Infection Biology, Spiering, Rachel, Wagenaar-Hilbers, Josée, Huijgen, Veerle, Van der Zee, Ruurd, Van Kooten, Peter J S, Van Eden, Willem, Broere, Femke, LS Immunologie, I&I RATIA-SIB, Strategic Infection Biology, Spiering, Rachel, Wagenaar-Hilbers, Josée, Huijgen, Veerle, Van der Zee, Ruurd, Van Kooten, Peter J S, Van Eden, Willem, and Broere, Femke

Published
2014

43. Identification of a novel kisspeptin with high gonadotrophin stimulatory activity in the dog

Author

CSCA AVM, Advances in Veterinary Medicine, I&I RATIA-SIB, Sub Voortplanting, Sub Endocrinologie, LS Immunologie, Onderzoek, Tissue Repair, CSCA TR1, Albers-Wolthers, Karin H J, de Gier, Jeffrey, Kooistra, Hans S, Rutten, Victor P M G, van Kooten, Peter J S, de Graaf, Janneke J, Leegwater, Peter A J, Millar, Robert P, Schaefers-Okkens, Auke C, CSCA AVM, Advances in Veterinary Medicine, I&I RATIA-SIB, Sub Voortplanting, Sub Endocrinologie, LS Immunologie, Onderzoek, Tissue Repair, CSCA TR1, Albers-Wolthers, Karin H J, de Gier, Jeffrey, Kooistra, Hans S, Rutten, Victor P M G, van Kooten, Peter J S, de Graaf, Janneke J, Leegwater, Peter A J, Millar, Robert P, and Schaefers-Okkens, Auke C

Published
2014

44. The immunostimulatory effect of CpG oligodeoxynucleotides on peripheral blood mononuclear cells of healthy dogs and dogs with atopic dermatitis

Author

Jassies-van der Lee, Annette, Rutten, Victor, Spiering, Rachel, van Kooten, Peter, Willemse, Ton, Broere, Femke, Sub Dermatologie, LS Immunologie, Risk Assessment of Toxic and Immunomodulatory Agents, and I&I RATIA-SIB

Subjects
Male, CpG Oligodeoxynucleotide, Regulatory T cell, Biology, T-Lymphocytes, Regulatory, Peripheral blood mononuclear cell, Dermatitis, Atopic, Dogs, Th2 Cells, Adjuvants, Immunologic, Interferon, medicine, Animals, Dog Diseases, RNA, Messenger, General Veterinary, Canine atopic dermatitis, TLR9, Interleukin, hemic and immune systems, Toll-like receptor 9, Th1 Cells, CpG-motif, veterinary(all), Interleukin-10, Interleukin 10, medicine.anatomical_structure, Gene Expression Regulation, Oligodeoxyribonucleotides, CpG site, Immunology, Leukocytes, Mononuclear, Cytokines, Female, Animal Science and Zoology, medicine.drug
Abstract

Synthetic oligodeoxynucleotides containing cytosine phosphatidyl guanine-rich DNA sequences (CpG ODN) can promote T-helper type 1 (Th1) responses, reduce T-helper type 2 (Th2) responses and/or favour regulatory T cell (Treg) responses in vitro and in vivo in humans and animals, by acting via Toll-like receptor 9 (TLR9). Since CpG ODN can be used as immune-modulators for canine atopic dermatitis (AD), the aim of the current study was to investigate their immunostimulatory potential on peripheral blood mononuclear cells (PBMC) and their subsets, from AD and healthy dogs. Expression of TLR9 and cytokine mRNA in CpG ODN-stimulated and unstimulated cells was assessed by real-time quantitative PCR. Stimulation of PBMC with CpG class C ODN upregulated mRNA expression of interleukin (IL)-6, interferon (IFN)-γ and IL-12p40 in AD dogs (P0.05). It also stimulated IFN-γ protein secretion by PBMC of atopic and healthy dogs as measured by ELISA. In healthy dogs only, CpG class C ODN stimulated IFN-α mRNA production by CD21(+) cells, and IL-10, IL-13 and IFN-γ mRNA production by CD3(+) cells. Increased expression of TLR9 mRNA was only observed in CD3(+) cells from AD dogs. No significantly increased gene expression was found in the CD11c(+) subset upon stimulation, for those genes evaluated. The results indicate that PBMC of healthy and atopic dogs are sensitive to stimulation with CpG ODN class C, with a resulting Th1 cytokine response in AD dogs and a mixed Th1/Th2/Treg cytokine response in healthy dogs. From this study, little evidence was found to support the use of CpG ODN class C for therapeutic purposes in dogs affected with AD.

Published
2014
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45. Identification of new populations of chicken natural killer (NK) cells

Author

Strategic Infection Biology, Dep Infectieziekten Immunologie, Jansen, C.A., van de Haar, P.M., van Haarlem, D.A., van Kooten, Peter, de Wit, Sjaak, van Eden, W., Viertlböck, B.C., Göbel, T.W., Vervelde, L., Strategic Infection Biology, Dep Infectieziekten Immunologie, Jansen, C.A., van de Haar, P.M., van Haarlem, D.A., van Kooten, Peter, de Wit, Sjaak, van Eden, W., Viertlböck, B.C., Göbel, T.W., and Vervelde, L.

Published
2010

46. Generation of the First TCR Transgenic Mouse with CD4+ T Cells Recognizing an Anti-inflammatory Regulatory T Cell-Inducing Hsp70 Peptide.

Author

Jansen, Manon A. A., van Herwijnen, Martijn J. C., van Kooten, Peter J. S., Hoek, Aad, van der Zee, Ruurd, van Eden, Willem, and Broere, Femke

Subjects
T cell receptors, AUTOIMMUNITY, ANTI-inflammatory agents
Abstract

Antigen-specific regulatory T cells (Tregs) directed at self-antigens are difficult to study since suitable specific tools to isolate and characterize these cells are lacking. A T cell receptor (TCR)-transgenic mouse would generate possibilities to study such antigen-specific T cells. As was shown previously, immunization with the mycobacterial heat shock protein (Hsp) 70-derived peptide B29 and its mouse homologs mB29a and mB29b induced anti-inflammatory responses. Furthermore, B29 induced antigen-specific Tregs in vivo. To study mB29b-specific Tregs, we isolated the TCR from T cell hybridomas generated against mB29b and produced a TCR transgenic mouse that expresses a MHC-class II restricted mB29b-specific TCR. These TCR transgenic CD4+ T cells were found to cross-react with the B29 epitope as identified with peptide-induced proliferation and IL-2 production. Thus, we have successfully generated a novel mouse model with antigen-specific CD4+ T cells that recognize self and bacterial Hsp 70-derived peptides. With this novel mouse model, it will be possible to study primary antigen-specific T cells with specificity for a regulatory Hsp70 T cell epitope. This will enable the isolation and characterization CD4+CD25+ Tregs with a proven specificity. This will provide useful knowledge of the induction, activation, and mode of action of Hsp70-specific Tregs, for instance, during experimental arthritis. [ABSTRACT FROM AUTHOR]

Published
2016
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