Your search keyword '"Arko Gorter"' showing total 3 results

1. Enhancement of the complement activating capacity of 17-1A mAb to overcome the effect of membrane-bound complement regulatory proteins on colorectal carcinoma

Author

Gert Jan Fleuren, Kyra A. Gelderman, Peter J. K. Kuppen, Wouter Bruin, and Arko Gorter

Subjects

Colorectal cancer, medicine.drug_class, medicine.medical_treatment, Immunology, CD59 Antigens, Biology, Monoclonal antibody, Membrane Cofactor Protein, Mice, Antigen, Antigens, CD, Antigens, Neoplasm, Tumor Cells, Cultured, medicine, Animals, Humans, Immunology and Allergy, Complement Activation, Elapid Venoms, Regulation of gene expression, Membrane Glycoproteins, CD55 Antigens, Antibodies, Monoclonal, Immunotherapy, Epithelial Cell Adhesion Molecule, medicine.disease, Molecular biology, Complement (complexity), Complement system, Complement C3b, Caco-2 Cells, Colorectal Neoplasms, Cell Adhesion Molecules, Adjuvant

Abstract

Adjuvant immunotherapy with 17-1A mAb directed against colorectal carcinoma is found to be effective in patients. However, 52 % of the patients treated with mAb 17-1A showed recurrence within 7 years. This high recurrence rate might be due to inhibition of complement activation by membrane-bound complement regulatory proteins (mCRP). The effect of these complement regulatory proteins might be reduced by blocking mCRP, or be overcome by activating more complement at the tumor cell membrane. In this study the complement-activating capacity of the 17-1A mAb was enlarged by conjugating it to cobra venom factor (CVF) or C3b. The most important C3 regulatory protein, CD55, was blocked using a bispecific mAb directed against the 17-1A / Ep-CAM antigen and CD55. Up to a 13-fold increase in C3 deposition was observed due to 17-1A-CVF and 17-1A-C3b, as compared to 17-1A. CD55 was shown to partly inhibit complement activation by these conjugates. The effect of the bispecific anti-17-1A / Ep-CAM*anti-CD55 mAb was compared with 17-1A conjugates with CVF or C3, and bispecific mAb were shown to be equally or more efficient in complement activation than the 17-1A-CVF or 17-1A-C3b conjugates. Therefore, 17-1A conjugates and anti-17-1A / EpCAM*anti-CD55 bispecific mAb may be promising immunotherapeutic agents for patients with colorectal cancer.

Published

2002

2. Cross-linking tumor cells with effector cells via CD55 with a bispecific mAb induces beta-glucan-dependent CR3-dependent cellular cytotoxicity

Author

Suzanne Lam, Arko Gorter, Cornelis F. M. Sier, and Kyra A. Gelderman

Subjects

Cytotoxicity, Immunologic, beta-Glucans, Immunology, Priming (immunology), Macrophage-1 Antigen, chemical and pharmacologic phenomena, Cell Communication, Biology, Antigen, Antigens, Neoplasm, Cell Line, Tumor, parasitic diseases, Antibodies, Bispecific, Immunology and Allergy, Humans, Cytotoxicity, Lymphokine-activated killer cell, CD55 Antigens, Effector, hemic and immune systems, Epithelial Cell Adhesion Molecule, Flow Cytometry, Molecular biology, Tumor antigen, Cell biology, Cross-Linking Reagents, biology.protein, iC3b, Antibody, Colorectal Neoplasms, Cell Adhesion Molecules

Abstract

Complement (C) regulatory proteins decrease the effectiveness of immunotherapeutic anti-cancer antibodies. Bispecific mAb (bi-mAb) that target a tumor antigen and simultaneously inhibit a C regulator increase the effectiveness of such a therapy. Here we investigated the mechanism by which bi-mAb increase tumor cell lysis. Apart from C-dependent cytotoxicity, C activation can lead to complement receptor 3 (CR3)-dependent cellular cytotoxicity (CR3-DCC) by CR3-positive effector cells in the presence of beta-glucan. Here we show that an anti-Ep-CAM*anti-CD55 bi-mAb induced more than threefold higher CR3-DCC (71%) of human colorectal cancer cells compared with anti-Ep-CAM alone (20%). This CR3-DCC was dependent on the binding of the anti-CD55 arm of tumor-bound anti-Ep-CAM*anti-CD55 bi-mAb to effector cell CD55, CR3 priming by beta-glucan and the presence of iC3b on the target cell. Comparable lysis could be obtained in the absence of iC3b, when CR3 and CD55 were cross-linked on the effector cells, suggesting cooperation between CD55 and CR3 in signal transduction. Tumor cells with low antigen expression were effectively lysed via this mechanism in contrast to direct C-dependent cytotoxicity. These data imply that the effectiveness of mAb immunotherapy can be improved using anti-tumor antigen*anti-CD55 bi-mAb and beta-glucan, thereby initiating CR3-DCC as an additional effector mechanism that is efficient for eradication of tumor cells with lower antigen expression.

Published

2006

3. Activation of the alternative pathway of complement by human serum IgA

Author

Arko Gorter, M. E. Stuurman, L. A. Van Es, Mohamed R. Daha, and Pieter S. Hiemstra

Subjects

Erythrocytes, Lysis, Complement Pathway, Alternative, Immunology, Succinimides, In Vitro Techniques, chemistry.chemical_compound, Animals, Humans, Immunology and Allergy, Complement Activation, Sheep, Properdin, biology, Complement C3, Molecular biology, Immune complex, Immunoglobulin A, Complement system, EGTA, Cross-Linking Reagents, Solubility, chemistry, Biochemistry, Polyclonal antibodies, biology.protein, Alternative complement pathway, Antibody, Protein Binding

Abstract

In order to study the activation of complement by soluble aggregates of human polyclonal serum IgA, lysis of sheep erythrocytes (E) coated with several IgA preparations was used as a model. A complement nonactivating monoclonal mouse IgG1 against IgA was used to coat the cells. IgA, isolated from normal human serum, was aggregated by either N-succinimidyl 3-(2-pyridyldithio)propionate (SPDP), glutaraldehyde, carbodiimide or heating. Depending on the size of the aggregates, and on the method of aggregation, E coated with aggregated IgA (E gamma 1.AIgA) could be lysed. The alternative pathway of complement appeared to mediate the lysis because the latter was observed in the presence of EGTA containing 5 mM Mg2+ (MgEGTA) and properdin (P) was deposited on the cells. Furthermore, no lysis was observed in C3-deficient serum. In the absence of AIgA the cells were not lysed, and no P deposition was observed. In another set of experiments E gamma 1.AIgA were first reacted with purified C3, B, D and P for 30 min at 30 degrees C, and subsequently in rat serum EDTA at 37 degrees C. Lysis occurred when E gamma 1.AIgA were prepared using SPDP-, glutaraldehyde- or carbodiimide-AIgA. Incubation of 100 micrograms/ml SPDP-AIgA with normal human serum for 30 min at 37 degrees C in the presence or absence of MgEGTA also induced consumption of total complement. The other soluble AIgA preparations were less effective in activating complement. These results suggest that polymeric serum IgA is capable of activating the alternative pathway of complement.

Published

1987