Your search keyword '"Szalai K"' showing total 4 results

1. Immunization with mimotopes prevents growth of carcinoembryonic antigen positive tumors in BALB/c mice.

Author

Brämswig KH, Knittelfelder R, Gruber S, Untersmayr E, Riemer AB, Szalai K, Horvat R, Kammerer R, Zimmermann W, Zielinski CC, Scheiner O, and Jensen-Jarolim E

Subjects

Animals, Antigens, Neoplasm chemistry, Drug Design, Enzyme-Linked Immunosorbent Assay, Epitopes chemistry, Glycoproteins chemistry, Immune System, Mice, Mice, Inbred BALB C, Microscopy, Fluorescence, Neoplasm Transplantation, Peptide Library, Peptides chemistry, Phylogeny, Carcinoembryonic Antigen chemistry, Gene Expression Regulation, Neoplastic, Immunotherapy methods

Abstract

Purpose: The carcinoembryonic antigen (CEA) is a glycoprotein that is overexpressed in nearly 50% of all human and veterinarian tumors. At present, anti-CEA antibodies are being tested in clinical studies as passive immunotherapeutics. This study aims to establish an active immunotherapy for the poorly immunogenic CEA glycoprotein by generating antigen surrogates., Experimental Design: We used the monoclonal anti-CEA antibody Col-1 and the biopanning method to generate peptide mimics (mimotopes) of the Col-1 epitope. The peptide showing the highest specificity and mimicry was synthesized as an octameric multiple antigenic mimotope (MAM). Subsequently, immunogenicity of the selected mimotope was examined in BALB/c mice. We assessed antibody-dependent cellular cytotoxicity and complement-dependent cytotoxicity mediated by the induced antibodies on CEA-expressing HT29 tumor cells. Furthermore, after immunization, the BALB/c mice were transplanted s.c. with Meth-A/CEA tumor cells., Results: When BALB/c mice were immunized with this MAM, they generated a specific humoral immune response against CEA. The mimotope-induced polyclonal and poly-isotypic antibodies induced antibody-dependent cellular cytotoxicity and complement-dependent cytotoxicity in vitro. Furthermore, when MAM-immunized mice were transplanted s.c. with Meth-A/CEA cells expressing human CEA, a suppressed tumor growth was observed., Conclusion: From our results, we can conclude that the Col-1 epitope of the glycoprotein CEA can be translated into an immunogenic peptide mimic. The mimotope-induced antibodies recognize CEA and do effectively inhibit growth of CEA-positive tumors. Based on these finding, we suggest that the generated mimotopes are candidates for active immunotherapy of CEA-expressing tumors.

Published

2007

2. Vaccination strategies based on the mimotope concept

Author

Szalai K, Erika Jensen-Jarolim, and Pali-Schöll I

Subjects

Epitopes, Vaccines, Vaccination, Humans, Immunotherapy, Forecasting

Abstract

Specific immunotherapies are in broad use for many diseases like allergies, cancer, autoimmune diseases or parasitic infections. Although clinical trials show successful application of these therapies, several disadvantages hinder the complete success. High production costs and repeated administrations represent the practical problems, while the possibly occurring side effects are the therapeutic troubles. To avoid these problems, the target specificity should be considered more intensely. Epitopes, the particular parts of antigens/allergens where they bind specific antibodies, are useful targets. To generate an epitope-specific vaccination, mimotopes can be identified via the biopanning technology. Mimotopes are small peptides mimicking the epitopes in the structural as well as in the immunological point of few. They are able to induce antigen-specific antibodies in active immunization form. These antibodies are directed against the natural antigen/allergen, and therefore they are able to block the outbreak of the diseases. Current research focuses on the development of mimotopes to achieve an epitope-specific induction of blocking antibodies, e.g. for allergy treatment. In cancer therapy, studies with mimotopes show successful interference with tumor cell growth in immunizations of mice. Also in the case of autoimmune diseases and parasitic infections this method was applied, targeting different molecules, which are key mediators in the disease mechanisms. Through the mimotope treatment via the specific antibody production, the disease symptoms could be hampered. This review gives an overview of the use of the mimotope concept and also of related therapeutic trials for the treatment of allergy, cancer, autoimmune and infectious diseases.

Published

2008

3. An unfolded variant of the major peanut allergen Ara h 2 with decreased anaphylactic potential.

Author

Starkl, P., Felix, F., Krishnamurthy, D., Stremnitzer, C., Roth-Walter, F., Prickett, S. R., Voskamp, A. L., Willensdorfer, A., Szalai, K., Weichselbaumer, M., O'Hehir, R. E., and Jensen-Jarolim, E.

Subjects

ALLERGIES, IMMUNOTHERAPY, IMMUNOLOGIC diseases, T cells, ENZYME-linked immunosorbent assay

Abstract

Background Peanut allergy causes severe type 1 hypersensitivity reactions and conventional immunotherapy against peanut allergy is associated with a high risk of anaphylaxis. Objective Our current study reports proof of concept experiments on the safety of a stably denatured variant of the major peanut allergen Ara h 2 for immunotherapy. We determined the impact of structure loss of Ara h 2 on its IgE binding and basophil degranulation capacity, T cell reactivity as well as anaphylactic potential. Methods The secondary structure of untreated and reduced/alkylated Ara h 2 variants was determined by circular dichroism spectroscopy. We addressed human patient IgE binding to Ara h 2 by ELISA and Western blot experiments. RBL- SX38 cells were used to test the degranulation induced by untreated and reduced/alkylated Ara h 2. We assessed the anaphylactic potential of Ara h 2 variants by challenge of sensitized BALB/c mice. T cell reactivity was investigated using human Ara h 2-specific T cell lines and splenocytes isolated from sensitized mice. Results Reduction/alkylation of Ara h 2 caused a decrease in IgE binding capacity, basophil degranulation and anaphylactic potential in vivo. However, the human T cell response to reduced/alkylated and untreated Ara h 2 was comparable. Mouse splenocytes showed higher metabolic activity upon stimulation with reduced/alkylated Ara h 2 and released similar IL-4, IL-13 and IFNγ levels upon treatment with either Ara h 2 variant. Conclusions and Clinical Relevance Reduced/alkylated Ara h 2 might be a safer alternative than native Ara h 2 for immunotherapeutic treatment of peanut allergic patients. [ABSTRACT FROM AUTHOR]

Published

2012

4. Mimotope vaccination for therapy of allergic asthma: anti-inflammatory effects in a mouse model.

Author

Wallmann, J., Epstein, M. M., Singh, P., Brunner, R., Szalai, K., El-Housseiny, L., Pali-Schöll, I., and Jensen-Jarolim, E.

Subjects

IMMUNOTHERAPY, POLLEN, ASTHMA, T cells, ALLERGENS, AEROSOLS, EPITOPES

Abstract

Background One of the concerns of allergen-specific immunotherapy is the possible boost of inflammatory allergen-specific T lymphocytes. To address this problem, treatment with B cell epitopes devoid of allergen-specific T cell epitopes would be a promising alternative. Objective In this study, we examined the therapeutic potency of a single mimotope, mimicking a structural IgE epitope of grass pollen allergen Phl p 5 in an established memory mouse model of acute allergic asthma. Methods In the experimental set-up, BALB/c mice were primed with intraperitoneal injections of recombinant Phl p 5a (rPhl p 5a) and subsequently aerosol challenged with the nebulized allergen. Mice developed signs of bronchial asthma including hypereosinophilia around bronchi, goblet cell hyperplasia and enhanced mucus production. Results When the mice were subsequently treated with the grass pollen mimotope coupled to keyhole limpet haemocyanin, bronchial eosinophilic inflammation and mucus hypersecretion decreased. Further, a decrease of Th2 cytokines IL-4 and IL-5 could be observed in the bronchoalveolar lavage (BAL). In contrast to rPhl p 5a, the mimotope was in vitro not able to stimulate splenocytes to proliferation or IL-5 production. Despite not affecting the levels of pre-existing IgE, vaccination with the single mimotope thus rendered anti-inflammatory effects in a mouse model of acute asthma. Conclusion From our data, we conclude that vaccination with a mimotope peptide representing a single IgE epitope of the allergen Phl p 5a and being devoid of allergen-specific T cell epitopes is able to down-regulate inflammation in acute asthma. Cite this as: J. Wallmann, M. M. Epstein, P. Singh, R. Brunner, K. Szalai, L. El-Housseiny, I. Pali-Schöll and E. Jensen-Jarolim, Clinical & Experimental Allergy, 2010 (40) 650–658. [ABSTRACT FROM AUTHOR]

Published

2010