Your search keyword '"van Gool, S"' showing total 23 results

1. A single-centre analysis of post-colonoscopy colorectal cancer.

Author

Aerts, R., Severi, C., Van Roey, G., Harlet, R., T’Syen, M., Claessens, C., Van Gool, S., Croonen, C., and Janssens, J.

Published

2021

2. Modelling greenhouse climate factors to constrain internal fruit rot (Fusarium spp.) in bell pepper.

Author

Frans, M., Moerkens, R., Van Gool, S., Sauviller, C., Van Laethem, S., Luca, S., Aerts, R., and Ceusters, J.

Subjects

FRUIT rots, BELL pepper, GREENHOUSE plants, CLIMATE in greenhouses, FUSARIUM, ATMOSPHERIC models

Abstract

Internal fruit rot in bell pepper is an important fungal disease which results in mycelium growth and/or necrosis on the ovarium and fruit flesh. It is mainly caused by members of the Fusarium lactis species complex and emerged as a major threat for bell pepper production worldwide. Infection already starts during anthesis, but the symptoms are only visible later on in the production chain. An accurate prediction of the disease incidence in the greenhouse based on environmental parameters is an important step towards a sustainable disease control. Based on a large dataset (2011-2016), a binomial, logistic regression model was developed. This model enables an accurate prediction of internal fruit rot occurrence based on simple and robust input parameters such as temperature and relative humidity during anthesis. Spore density was included as a simplified, practical parameter describing the presence or absence of internal fruit rot 1 week earlier. The obtained model was validated with an independent dataset of five different commercial bell pepper greenhouses. The chance of internal fruit rot infection increased with temperature and relative humidity. Once a greenhouse is infected, only lower temperatures can reduce future risks. However, the chance of the disease to occur remains very high. This prediction model offers a strong instrument for growers to optimize greenhouse climate conditions to restrain internal fruit rot incidence. In addition, the model can be used to apply accurate biological or chemical treatments to achieve a more sustainable greenhouse control. A guideline table for climate adjustment is presented. [ABSTRACT FROM AUTHOR]

Published

2018

3. A case of amoebic colitis with amoeboma and simultaneous liver abscesses. A diagnosis by colonoscopy.

Author

Bronswijk, M. and Van Gool, S.

Published

2019

4. Gremlin 1, frizzled-related protein, and Dkk-1 are key regulators of human articular cartilage homeostasis.

Author

Leijten, J. C. H., Emons, J., Sticht, C., Van Gool, S., Decker, E., Uitterlinden, A., Rappold, G., Hofman, A., Rivadeneira, F., Scherjon, S., Wit, J. M., Van Meurs, J., Van Blitterswijk, C. A., and Karperien, M.

Subjects

CARTILAGE physiology, ACADEMIC medical centers, ANALYSIS of variance, CELLULAR signal transduction, CONFIDENCE intervals, STATISTICAL correlation, EPIDEMIOLOGY, GENETIC polymorphisms, IMMUNOHISTOCHEMISTRY, OSTEOARTHRITIS, POLYMERASE chain reaction, RESEARCH funding, GENOMICS, DATA analysis, EQUIPMENT & supplies, REVERSE transcriptase polymerase chain reaction, DATA analysis software, CHILDREN

Abstract

Objective The development of osteoarthritis (OA) may be caused by activation of hypertrophic differentiation of articular chondrocytes. Healthy articular cartilage is highly resistant to hypertrophic differentiation, in contrast to other hyaline cartilage subtypes, such as growth plate cartilage. The purpose of this study was to elucidate the molecular mechanism responsible for the difference in the propensity of human articular cartilage and growth plate cartilage to undergo hypertrophic differentiation. Methods Whole-genome gene-expression microarray analysis of healthy human growth plate and articular cartilage derived from the same adolescent donors was performed. Candidate genes, which were enriched in the articular cartilage, were validated at the messenger RNA (mRNA) and protein levels and examined for their potential to inhibit hypertrophic differentiation in two models. In addition, we studied a possible genetic association with OA. Results Pathway analysis demonstrated decreased Wnt signaling in articular cartilage as compared to growth plate cartilage. This was at least partly due to increased expression of the bone morphogenetic protein and Wnt antagonists Gremlin 1, Frizzled-related protein (FRP), and Dkk-1 at the mRNA and protein levels in articular cartilage. Supplementation of these proteins diminished terminal hypertrophic differentiation without affecting chondrogenesis in long-bone explant cultures and chondrogenically differentiating human mesenchymal stem cells. Additionally, we found that single-nucleotide polymorphism rs12593365, which is located in a genomic control region of GREM1, was significantly associated with a 20% reduced risk of radiographic hip OA in 2 population-based cohorts. Conclusion Taken together, our study identified Gremlin 1, FRP, and Dkk-1 as natural brakes on hypertrophic differentiation in articular cartilage. As hypertrophic differentiation of articular cartilage may contribute to the development of OA, our findings may open new avenues for therapeutic intervention. [ABSTRACT FROM AUTHOR]

Published

2012

5. Dysphagia lusoria caused by a right-sided aorta.

Author

De Caluwe, E., Verhaegen, S., Van Roey, G., Janssens, J., and Van Gool, S.

Published

2012

6. Wilms’ tumour gene 1 (WT1) positivity in endothelial cells surrounding epithelial uterine tumours.

Author

Coosemans, A., Van Hove, Th., Verbist, G., Moons, L., Neven, P., Moerman, Ph., Vergote, I., Van Gool, S. W., and Amant, F.

Subjects

LETTERS to the editor, NEPHROBLASTOMA

Abstract

A letter to the editor is presented regarding the positivity of Wilms' tumour gene 1 in endothelial cells that surround epithelial uterine tumours.

Published

2009

7. Influence of intrapyloric botulinum toxin injection on gastric emptying and meal-related symptoms in gastroparesis patients.

Author

ARTS, J., VAN GOOL, S., CAENEPEEL, P., VERBEKE, K., JANSSENS, J., and TACK, J.

Subjects

BOTULINUM toxin, NAUSEA, GASTROINTESTINAL diseases, INDIGESTION, DOMPERIDONE, PYLORUS, ENDOSCOPY

Abstract

Background Recent observations in limited numbers of patients suggest a potential benefit of intrapyloric injection of botulinum toxin in the treatment of gastroparesis. Aim To characterize the effect of botulinum toxin on solid and liquid gastric emptying and on meal-related symptoms. Methods In 20 gastroparesis patients (17 women, mean age 37 ± 3 years, three diabetic and 17 idiopathic), gastric emptying for solids and liquids was measured before and one month after intrapyloric botulinum toxin 4 × 25 units. Before the meal and at 15-min intervals up to 240 min postprandially, the patient graded the intensity of six gastroparesis symptoms, and a meal-related severity score was obtained by adding all intensities. Data (mean ± S.E.M.) were compared using paired Student's t-test. Results Treatment with botulinum toxin significantly enhanced solid ( t1/2 132 ± 16 vs. 204 ± 35 min, P < 0.05) but not liquid (92 ± 10 vs. 104 ± 11 min, N.S.) emptying. This was accompanied by a significant decrease in cumulative meal-related symptom score (73.5 ± 16.3 vs. 103 ± 17.1 baseline, P = 0.01) as well as individual severity scores for postprandial fullness, bloating, nausea and belching (all P < 0.001, two-wayanova). Conclusions Botulinum toxin improves solid but not liquid gastric emptying in gastroparesis, and this is accompanied by significant improvement of several meal-related symptoms. [ABSTRACT FROM AUTHOR]

Published

2006

8. Surgery and adjuvant dendritic cell-based tumour vaccination for patients with relapsed malignant glioma, a feasibility study.

Author

Rutkowski, S., De Vleeschouwer, S., Kaempgen, E., Wolff, J. E. A., Kühl, J., Demaerel, P., Warmuth-Metz, M., Flamen, P., Van Calenbergh, F., Plets, C., Sörensen, N., Opitz, A., Van Gool, S. W., Kühl, J, and Sörensen, N

Subjects

CANCER patients, TUMOR surgery, DENDRITIC cells, VACCINATION, CANCER relapse, GLIOMAS, GLIOMA treatment, DELAYED hypersensitivity, PILOT projects, RESEARCH, IMMUNIZATION, RESEARCH methodology, IMMUNOMODULATORS, EVALUATION research, COMPARATIVE studies, CANCER vaccines, COMBINED modality therapy, CEREBRAL edema

Abstract

Patients with relapsed malignant glioma have a poor prognosis. We developed a strategy of vaccination using autologous mature dendritic cells loaded with autologous tumour homogenate. In total, 12 patients with a median age of 36 years (range: 11-78) were treated. All had relapsing malignant glioma. After surgery, vaccines were given at weeks 1 and 3, and later every 4 weeks. A median of 5 (range: 2-7) vaccines was given. There were no serious adverse events except in one patient with gross residual tumour prior to vaccination, who repetitively developed vaccine-related peritumoral oedema. Minor toxicities were recorded in four out of 12 patients. In six patients with postoperative residual tumour, vaccination induced one stable disease during 8 weeks, and one partial response. Two of six patients with complete resection are in CCR for 3 years. Tumour vaccination for patients with relapsed malignant glioma is feasible and likely beneficial for patients with minimal residual tumour burden. [ABSTRACT FROM AUTHOR]

Published

2004

9. Blocking B7 and CD40 co-stimulatory molecules decreases antiviral T cell activity.

Author

Vermeiren, J., Ceuppens, J. L., Haegel-Kronenberger, H., De Boer, M., Boon, L., and Van Gool, S. W.

Subjects

IMMUNE system, GRAFT rejection, GREEN fluorescent protein, T cells, CD antigens, ADENOVIRUSES, TRANSGENIC mice, CYTOKINES, INTERFERONS

Abstract

Inhibition of co-stimulatory signals for T cells by interrupting CD80/CD86–CD28 and CD40–CD154 interactions is a promising approach to prevent transplant rejection and to induce graft tolerance. However, this tolerizing treatment might affect T cell reactivity towards all the antigens to which the immune system is exposed during treatment. We addressed the question whether such inhibition of co-stimulatory ligands on human antigen presenting cells (APC) would affect T cell reactivity against a virus. This was tested in an in vitro system with freshly isolated human monocytes transduced with adenovirus (ad) containing either murine interferon- γ (mIFN- γ) or green fluorescent protein (GFP) as marker transgene. T cells co-cultured with transduced monocytes proliferated and produced cytokines. These ‘primed’ T cells had strong antiviral activity as they subsequently killed ad/GFP-transduced monocytes and reduced mIFN- γ accumulation in coculture with ad/mIFN-transduced monocytes. However, if priming had occurred in the presence of blocking anti-CD40/CD80/CD86 MoAbs, generation of this antiviral activity was completely prevented. Moreover, T cells primed in the absence of co-stimulatory cells failed to proliferate upon restimulation with adenovirus-transduced monocytes. The results confirm that co-stimulatory signals from APC are required for efficient induction of antiviral T cell activity and point to a potential infectious risk of blocking co-stimulatory signals. [ABSTRACT FROM AUTHOR]

Published

2004

10. Regulation of the IL-10 Production by Human T Cells.

Author

Rafiq, K., Charitidou, L., Bullens, D. M. A., Kasran, A., Lorré, K., Ceuppens, J. L., and Van Gool, S. W.

Subjects

INTERLEUKIN-10, MONOCYTES, MACROPHAGES, B cells

Abstract

Interleukin (IL)-10, an immunomodulatory cytokine predominantly produced by monocytes/macrophages and T cells, inhibits several functions of dendritic cells (DC), monocytes and T cells including their cytokine production, but it stimulates B cell immunoglobulin (Ig) production and cytotoxic T lymphocyte (CTL) generation. A precise knowledge of the mechanisms that control the IL-10 production is therefore highly important for understanding the immunoregulation. The IL-10 production was studied in cultures of freshly isolated human T cells. A rise in intracellular calcium as well as the common γ-chain containing cytokine receptor triggering or CD28 triggering were found to be important signals for IL-10 induction. CD80, CD58, rIL-12 and rIFN-α all had efficacious and independent costimulatory activities on the IL-10 production, while PGE2 was inhibitory. Dependence on autocrine IL-2 signalling was shown by the effects of anti-IL-2 and anti-IL-2R monoclonal antibodies (MoAb), but the IL-10 production proceeded partly IL-2-independent when CD80 provided costimulation. Sensitivity to inhibition by CsA was not removed by CD80 or CD58 costimulation and/or by addition of rIL-12 or rIFN-α, pointing to the absolute requirement for calcineurin activity. These data reveal important differences in the regulatory pathways between IL-10 (a cytokine-inhibitory interleukin) and IL-2 (a cytokine-inducing interleukin), which can potentially be exploited therapeutically. The fact that CsA blocks the production of IL-10, which itself has important immunosuppressive properties, should be taken into account in defining immunosuppressive treatment schedules which include the use of CsA. [ABSTRACT FROM AUTHOR]

Published

2001

11. Disease- and treatment-related elevation of the neurodegenerative marker tau in children with hematological malignancies.

Author

Van Gool, S W, Van Kerschaver, E, Brock, P, Pottel, H, Hulstaert, F, Vanmechelen, E, Uyttebroeck, A, Van De Voorde, A, and Vanderstichele, H

Subjects

LEUKEMIA, NEUROTOXICOLOGY, CEREBROSPINAL fluid

Abstract

Children acquire neuropsychologic dysfunctions after chemotherapy for hematologic malignancy. In this study, putative changes in levels of CSF-tau (a marker of neural dysintegrity) in leukemic children prior to and during chemotherapy were studied. Cerebrospinal fluid (CSF) samples were obtained before and during treatment from patients with B cell non-Hodgkin's lymphoma (NHL, n = 10), non-B cell acute lymphoblastic leukemia/NHL (non-B-ALL, n = 48), acute myeloid leukemia (AML, n = 9), other malignant diseases (n = 9), and six control children. A sandwich-type ELISA (INNOTEST hTAU-Ag) was used for measuring CSF-tau. Sixteen out of 50 patients with hematological malignancies, including the patients with proven leukemic CNS invasion, already showed high CSF-tau levels at baseline (>300 pg/ml). The pre-induction treatment for non-B-ALL, consisting of only corticosteroids and methotrexate (MTX), resulted in a significant increase of tau at day 8 (on average to 535 pg/ml). Larger increases as compared to baseline levels of CSF-tau were observed in patients treated for B-NHL with systemic vincristine, corticosteroids and cyclophosphamide, and intrathecal MTX (mean 776 pg/ml at day 8). In two AML patients with CNS invasion, CSF-tau increased during chemotherapy up to 1,500 and 948 pg/ml, respectively. In one non-B-ALL patient with MTX-induced clinical neurotoxicity, CSF-tau was above the detection limit of 2,000 pg/ml. Almost one-third of the patients with hematological malignancies had elevated CSF-tau levels at diagnosis. Transient high levels of CSF-tau, reaching levels observed in other neurodegenerative disorders, were observed during induction chemotherapy for non-B-ALL, B-NHL and CNS+ AML. The clinical implications of both observations will be the subject of further study. [ABSTRACT FROM AUTHOR]

Published

2000

12. Interaction of CTLA‐4 (CD152) with CD80 or CD86 inhibits human T‐cell activation.

Author

Vandenborre, K., Van Gool, S. W., Kasran, A., Ceuppens, J. L., Boogaerts, M. A., and Vandenberghe, P.

Subjects

ANTIGENS, MICE, T cells

Abstract

Summary Occupancy of CTLA‐4 (cytotoxic T‐lymphocyte antigen‐4 or CD152) negatively regulates the activation of mouse T lymphocytes, as indicated by the fate of CTLA‐4‐deficient mice, by the impact of anti‐CTLA‐4 monoclonal antibodies (mAbs) on mouse T‐cell activation in vitro and by the impact of CTLA‐4 blockade on the course of experimental tumoral, autoimmune, alloimmune or infectious disease in this animal. The function of human CTLA‐4, however, remains less clear. The expression and function of human CTLA‐4 were further explored. CTLA‐4 was expressed under mitogenic conditions only, its expression being, at least partially, dependent on the secretion of interleukin‐2. Memory T cells expressed CTLA‐4 with faster kinetics than naive T cells. The functional role of human CTLA‐4 was assessed utilizing a panel of four anti‐CTLA‐4 mAbs that blocked the interaction between CTLA‐4 and its ligands. These mAbs, in immobilized form, profoundly inhibited the activation of T cells by immobilized anti‐CD3 mAb in the absence of anti‐CD28 mAb, but co‐stimulated T‐cell activation in the presence of anti‐CD28 mAb. Finally, and importantly, blockade of the interaction of CTLA‐4 with its ligands using soluble anti‐CTLA‐4 mAbs, in intact form or as Fab fragments, enhanced T‐cell activation in several polyclonal or alloantigen‐specific CD80‐ or CD80/CD86‐dependent assays, as measured by cytokine production, cellular proliferation or cytotoxic responses. It is concluded that interaction of CTLA‐4 with its functional ligands, CD80 or CD86, can down‐regulate human T‐cell responses, probably by intracellular signalling events and independent of CD28 occupancy. [ABSTRACT FROM AUTHOR]

Published

1999

13. CD57+/CD28- T cells in untreated hemato-oncological patients are expanded and display a Th1-type cytokine secretion profile, ex vivo cytolytic activity and enhanced tendency to apoptosis.

Author

Van den Hove, L E, Van Gool, S W, Vandenberghe, P, Boogaerts, M A, and Ceuppens, J L

Subjects

CYTOKINES, T cells, APOPTOSIS

Abstract

Three-color flow cytometry immunophenotyping revealed significant increases of CD57+ and CD28- cells among both circulating CD4+ and CD8+ T lymphocytes of untreated hemato-oncological patients (n = 54) as compared to healthy donors (n = 55), with CD57 and CD28 expression on the patients' T cells being largely reciprocal. Marked expansion of CD57+ cells among circulating CD4+ T lymphocytes was frequently detected in patients with chronic leukemia of B cell origin (B-CLL, hairy cell leukemia) but not in patients with chronic myeloid leukemia, suggesting a causal relation with the tumor's major histocompatibility complex class II expression. Using immunomagnetic separation techniques, we further demonstrate that the patients' CD57+/CD28- T cells display a typical Th1-type cytokine secretion profile upon anti-CD3 stimulation, with a markedly higher secretion of the Th1-type cytokines IL-2, IFN-gamma, and TNF-alpha than their CD57-/CD28+ counterparts. Cytotoxic activity of circulating CD8+ T lymphocytes, measured ex vivo in an anti-CD3-redirected assay, was almost exclusively exerted by the CD57+/CD28- subset. Moreover, a marked cytotoxic activity was detected within CD4+CD57+ T cells from some B-CLL patients. Finally, the patients' CD57+/CD28- T cells displayed an increased tendency to apoptosis in culture. Collectively, our results indicate that the expanded CD57+/CD28- T cells in hemato-oncological patients represent differentiated effector cells, similar to their (quantitatively minor) counterpart in healthy donors. The reason for their expansion and their pathophysiologic significance, however, remains unclear. [ABSTRACT FROM AUTHOR]

Published

1998

14. Expression of B7-2 (CD86) molecules by Reed-Sternberg cells of Hodgkin's disease.

Author

Van Gool, S W, Delabie, J, Vandenberghe, P, Coorevits, L, De Wolf-Peeters, C, and Ceuppens, J L

Subjects

HODGKIN'S disease, TUMOR immunology, T cells

Abstract

Ligation of CD28 on T cells with its natural ligands B7-1 (CD80) or B7-2 (CD86) provides a major costimulatory signal for T cells and is of potential importance for tumor rejection. We previously reported a strong expression of B7-1 on Reed-Sternberg cells and anaplastic large cell lymphoma cells. We report here our findings on B7-2 expression by malignant lymphomas (n = 70). B7-2 was present on the neoplastic cells of anaplastic large cell lymphoma in two of three cases studied, and on a subpopulation of the malignant cells in one out of four cases of follicular lymphoma. B7-2 was not expressed by the neoplastic cells of the other non-Hodgkin's lymphomas (n = 32), including T cell-rich B cell lymphoma. In contrast, Reed-Sternberg cells in lymph nodes affected by Hodgkin's disease are strongly positive for B7-2 (n = 31). Evidence for a functional correlate of this expression was obtained by our findings that the combination of anti-B7-1 and anti-B7-2 monoclonal antibodies was more effective than each separately in blocking allogeneic T cell activation (proliferation and cytokine secretion) by Hodgkin's disease-derived cell lines as stimulators. The possible role of B7-1 and B7-2 expression for the course and symptomatology of Hodgkin's disease is discussed. [ABSTRACT FROM AUTHOR]

Published

1997

15. CD40 triggering of chronic lymphocytic leukemia B cells results in efficient alloantigen presentation and cytotoxic T lymphocyte induction by up-regulation of CD80 and CD86 costimulatory molecules.

Author

Van den Hove, L E, Van Gool, S W, Vandenberghe, P, Bakkus, M, Thielemans, K, Boogaerts, M A, and Ceuppens, J L

Subjects

LYMPHOCYTIC leukemia, B cells

Abstract

Freshly collected chronic lymphocytic leukemia B cells (B-CLL cells) are known to be inefficient at stimulating allogeneic T cells, and to lack significant expression of B7 (CD80 and CD86) costimulatory molecules. We investigated the potential of CD40 triggering to up-regulate the expression of adhesion and costimulatory molecules on B-CLL cells, and to enhance their immunogenicity towards allogeneic T cells. B-CLL cells cocultured with human CD40 ligand-expressing mouse fibroblasts rapidly up-regulated CD54 and CD58 adhesion molecules and B7-1 (CD80) and B7-2 (CD86) costimulatory molecules, and acquired a strong stimulatory capacity towards CD4+ as well as isolated CD8+ allogeneic T cells. Costimulation by both CD80 and CD86 proved critical for allogeneic T cell proliferation and CD25 and HLA-DR expression, since these were strongly inhibited by anti-CD80 or anti-CD86 monoclonal antibodies, and completely abrogated by CTLA4-Ig fusion protein, which blocks both CD80 and CD86. B7 costimulation also proved critical for restimulation of primed B-CLL-reactive T cells. Most importantly, priming of purified CD8+ T cells with CD40-triggered allogeneic B-CLL cells resulted in cytotoxic activity against the unstimulated B-CLL cells. These findings raise the possibility that CD40 triggering of B-CLL cells might be exploited in immunotherapeutic protocols. [ABSTRACT FROM AUTHOR]

Published

1997

16. Accessory Signalling by B7-1 for T Cell Activation Induced by Anti-CD2: Evidence for IL-2-Independent CTL Generation and CsA-Resistant Cytokine Production.

Author

Van Gool, S. W., Kasran, A., Wallays, G., De Boer, M., and Ceuppens, J. L.

Subjects

T cells, ANTIGEN presenting cells, FIBROBLASTS, CELL proliferation, CYTOKINES, LYMPHOCYTES

Abstract

Resting T cells can be activated by selected pairs of anti-CD2 MoAb. Activation is dependent on the presence of accessory cells, which can be replaced by either anti-CD28, or by the combination of IL-1β and IL-6. The present study was undertaken to investigate accessory signalling by B7-1, the natural ligand of CD28, in this pathway of T cell activation. 3T6 mouse fibroblasts were transfected with human B7-1 and used as accessory cells in cultures of purified resting human T cells. In the presence of a stimulating pair of anti-CD2 MoAb, T cell proliferation, production of cytokines (IL-2, IL-4, IL-10, GM-CSF, IFN-γ and TNF-α), and generation of cytotoxic T lymphocytes were all supported by B7-1(+) 3T6 cells but not by control 3T6 cells. Blocking studies with anti-IL-2 + anti-IL-2R MoAb revealed both IL-2-dependent and IL-2-independent CTL generation after B7-1-mediated costimulation. Moreover, a partial or complete resistance to inhibition with CsA was observed for IL-2 production and CTL generation respectively in the presence of the costimulatory signal derived from B7-1 - CD28 interaction. Anti-CD2 MoAb with B7-1 costimulation could directly induce proliferation, IL-2 production and generation of CTL activity in highly purified CD8+ T cells without the help of CD4+ T cells. We conclude that CD28 ligation with the natural ligand B7-1 provides a strong accessory signal for CD4 and CD8 cell activation through CD2. [ABSTRACT FROM AUTHOR]

Published

1995

17. Production of granulocyte-macrophage colony-stimulating factor by T cells is regulated by B7 and IL-1β.

Author

Kruger, M., Van Gool, S., Peng, X.H., Coorevits, L., Casteels-van Daele, M., and Ceuppens, J. L.

Subjects

GRANULOCYTE-macrophage colony-stimulating factor, T cells, MONOCLONAL antibodies, CYTOKINES, INTERLEUKIN-1, IMMUNOLOGY

Abstract

Granulocyte-macrophage colony-stimulating factor (GM-CSF) has proliferation- and differentiation-inducing effects on immature myeloid cells in the bone marrow, and it can modulate the function of several types of mature myeloid cells. We have stimulated purified human T cells with immobilized anti-CD3 or mitogenic anti-CD2 (a combination of monoclonal antibodies 9-1 and 9.6) which could induce GM-CSF production. The cytokines interleukin-1β (IL-1β) and IL-2 strongly enhanced GM-CSF production, while IL-4, IL-6, GM-CSF, interferon-γ (IFN-γ) and turnout necrosis factor (TNF) had no effect. Activation of protein kinase C by phorbol myristate acetate or triggering of CD28 on T cells by monoclonal antibody 9.3 provided accessory signals for enhanced GM-CSF production in activated T cells. Most important, the addition of mouse cells transfected with human B7-1 (CD80), a natural ligand for CD28, provided a potent accessory signal for GM-CSF production by activated T cells, which could not be blocked by cyclosporin A. The effect of IL-1β was in fact indirect, and resulted from enhanced IL-2 production, while the effect of B7 resulted from both IL-2-dependent and IL-2-independent pathways. We conclude that antigen-presenting cells (APC) can up-regulate GM-CSF production through IL-1β and through CD28 triggering by B7 molecules. As GM-CSF itself up-regulates B7 expression and IL-1β production by APC, a bidirectional regulatory feedback pathway between APC and T cells seems to modulate GM-CSF production. [ABSTRACT FROM AUTHOR]

Published

1996

18. Phenotype, cytokine production and cytolytic capacity of fresh (uncultured) tumour-infiltrating T lymphocytes in human renal cell carcinoma.

Author

van Den Hove, L. E., van Gool, S. W., van Poppel, H., Baertt, L., Coorevits, L., van Damme, B., and Ceuppens, J. L.

Subjects

RENAL cell carcinoma, CYTOKINES, T cells, TUMOR necrosis factors, TUMOR immunology, IMMUNE response

Abstract

We investigated the phenotype and functional capacities of tumour-infiltrating lymphocytes (TIL). freshly isolated from primary renal cell carcinoma (RCC) specimens (n = 20). Three-colour flow cytometry immunophenotyping revealed that RCC TIL consist mainly of CD3 + T cells, with a clear predominance of CD4 -CD8 + over CD4+ CD8 - T cells, and a marked population of CD4 + CD8 + T cells. Natural killer (NK) cells were also strongly represented (> 25% in 15 of 20 tumour samples), while B cells constituted a minor TIL subset (< 5% in 18 of 20 tumour samples). More importantly, the T and NK cells within the tumour displayed a significantly higher expression of the early activation marker CD69 than their counter parts in adjacent normal renal tissue and in peripheral blood. Expression of CD54 and of HLA-DR was also elevated on CD3 + TIL. and HLA-DR expression was further vigorously up-regulated following ex vivo stimulation with anti-CD3, all suggesting enhanced immune activity within the tumour microenvironment, CD3 + CD4 + TIL displayed a normal capacity to up-regulate CD25 expression and to secrete both Thl-type (IL-2, tumour necrosis factor-alpha (TNF-α) and interferon-gamma (IFN-γ) and Th2-type (IL-4, IL-5 and IL-10) cytokines upon triggering with anti- CD3. Furthermore, cytokine production was susceptible to modulation by CD28 costimulation. CD3 + CD8 + TIL, on the other hand, consistently demonstrated a poor up-regulation of CD25 upon triggering with anti-CD3, and displayed poor ex vivo cytolytic activity in an anti-CD3-redirected 4-h cytotoxicity assay against murine P815 cells. Collectively, our findings indicate that the CD3 + CD4 + TIL in RCC have normal functional capacities, whereas the proportionally major CD3 + CD4 + TIL are functionally impaired. The relevance of these findings to the in vivo local immune response in RCC is discussed. [ABSTRACT FROM AUTHOR]

Published

1997

19. T Helper-Independent Activation of Human CD8+ Cells: the Role of CD28 Costimulation.

Author

Van Gool, S. W., Yiqun Zhang, Kasran, A., De Boer, M., and Ceuppens, J. L.

Subjects

MHC antibodies, CELLS, T cells, ANTIGEN presenting cells, MICE

Abstract

The concept that activation of MHC class I-restricted CD8+ cells entirely depends on help from MHC class II-restricted CD4+ T cells has recently been supplemented with an alternative model in which CD8+ cells can directly be activated by MHC class I-expressing professional antigen-presenting cells (APC), which are able to deliver an accessory signal. The authors analysed the role of CD28-mediated costimulation for T helper cell-independent activation of purified human CD8+ T cells in two different in vitro models. Freshly isolated CD8+ cells could be activated (proliferation, IL-2 production and cytotoxic activity) by anti-CD3-presenting FcγR+ mouse cells transfected with the human CD28 ligand, CD80, as the only accessory signal. On the other hand, activation of CD8+ cells by allogeneic MHC class I on EBV-transformed B cells, which express two different CD28 ligands, CD80 and CD86, also proceeded very efficiently (proliferation, cytotoxic activity and CD25 expression), but was either not, or only partially, blocked by anti-CD80 and anti-CD86 MoAb or CTLA-4Ig. This indicates that other costimulatory signals are also effective, and that CD28 triggering is not absolutely required for initial T-cell activation. CsA and CD80/CD86-blocking agents were synergistic in completely inhibiting activation of CD8+ cells in the MLR with allogeneic B-cell lines. This combination also induced non-responsiveness of CD8+ cells upon restimulation in the absence of blocking agents. Therefore, although professional APC can apparently provide multiple costimulatory signals for direct activation of CD8+ T cells, the signal derived from CD80/CD86 is unique in providing CsA-resistance. [ABSTRACT FROM AUTHOR]

Published

1996

20. Lacrimal gland and perioptic nerve lesions due to Langerhans cell histiocytosis (2007: 9b).

Author

Herman, M., Demaerel, P., Wilms, G., Gool, S., Casteels, I., and Van Gool, S

Subjects

PATIENTS, LACRIMAL apparatus, LANGERHANS cells, LANGERHANS-cell histiocytosis, CELL proliferation, METAPLASTIC ossification

Abstract

We report a patient presenting with bilateral lacrimal gland involvement and perioptic nerve sheath lesions due to Langerhans cell histiocytosis (LCH) invasion. LCH is a rare multisystemic disease characterized by a clonal proliferation of Langerhans cells. All organs may be involved with a clinical spectrum ranging from a solitary bone lesion to a severe life-threatening multisystem disease. Osteolytic orbital bone lesions with extension into the adjacent orbital soft tissues have been described. To our knowledge, lacrimal gland involvement has probably been described only once before. Perioptic nerve lesions are also very rare, having been described only three times before. [ABSTRACT FROM AUTHOR]

Published

2007

21. Successful treatment of recurrent thrombotic thrombocytopenic purpura with plasmapheresis and vincristine.

Author

Van Gool, S, Brock, P, Van Laer, P, Van Damme-Lombaerts, R, Proesmans, W, and Casteels-Van Daele, M

Abstract

An adolescent girl with severe thrombotic thrombocytopenic purpura (TTP) remained in a critical condition after 3 weeks of combined treatment with antiplatelet drugs, plasma infusions and plasma exchange. The introduction of vincristine resulted in gradual improvement and eventual complete remission which lasted for 2 years. When she relapsed, immediate improvement was observed with the combined treatment of plasmapheresis and vincristine. She has now been in complete remission again for 10 months. It is suggested that plasmapheresis plus vincristine should be used as the initial treatment for children with TTP. [ABSTRACT FROM AUTHOR]

Published

1994

22. Polyclonal immunoglobulins for intravenous use induce interleukin 10 release in vivo and in vitro.

Author

Lories, R. J., Daele, M. Casteels-Van, Ceuppens, J. L., and Van Gool, S. W.

Published

2004

23. Alobar holoprosencephaly, diabetes insipidus and coloboma without craniofacial abnormalities: a case report.

Author

Van Gool, S, de Zegher, F, de Vries, L S, Vanderschueren-Lodeweyckx, M, Devlieger, H, Casaer, P, and Eggermont, E

Subjects

BRAIN abnormalities, COMPARATIVE studies, IRIS (Eye), RESEARCH methodology, COLOBOMA, MEDICAL cooperation, RESEARCH, EVALUATION research, DIABETES insipidus, MULTIPLE human abnormalities, DISEASE complications

Abstract

An infant is described with coloboma of the right eye, holoprosencephaly and diabetes insipidus without craniofacial malformations. The association is discussed in view of the development of the prosencephalon and its relation to the development of craniofacial structures. [ABSTRACT FROM AUTHOR]

Published

1990