Your search keyword '"Fiebig, H."' showing total 8 results

1. Vaccines for birch pollen allergy based on genetically engineered hypoallergenic derivatives of the major birch pollen allergen, Bet v 1.

Author

Mahler V, Vrtala S, Kuss O, Diepgen TL, Suck R, Cromwell O, Fiebig H, Hartl A, Thalhamer J, Schuler G, Kraft D, and Valenta R

Subjects

Allergens genetics, Allergens toxicity, Animals, Antigens, Plant, Enzyme-Linked Immunosorbent Assay methods, Female, Genetic Engineering, Hypersensitivity immunology, Immunoglobulin E blood, Immunoglobulin G blood, Male, Mice, Mice, Inbred BALB C, Plant Proteins genetics, Vaccines, Synthetic administration & dosage, Vaccines, Synthetic genetics, Vaccines, Synthetic toxicity, Allergens administration & dosage, Allergens immunology, Hypersensitivity prevention & control, Immunotherapy methods, Plant Proteins immunology

Abstract

Background: We have recently engineered recombinant derivatives of the major birch pollen allergen Bet v 1 (rBet v 1 fragments and trimer) with strongly reduced allergenic activity., Objective: The aim of this study was the in vivo characterization of potential allergy vaccines based on Al(OH)3-adsorbed genetically modified rBet v 1 derivatives in mice., Methods: BALB/c mice were immunized either with courses of nine injections of increasing doses of Al(OH)3-adsorbed rBet v 1 wild-type, rBet v 1 fragments, rBet v 1 trimer or Al(OH)3 alone in weekly intervals or with three high-dose injections applied in intervals of 3 weeks. Humoral immune responses to rBet v 1 wild-type and homologous plant allergens were measured by ELISA and Western blotting, and the ability of mouse antibodies to inhibit the binding of allergic patients IgE to Bet v 1 was studied by ELISA competition experiments., Results: In both schemes, hypoallergenic rBet v 1 derivatives induced low IgE but high IgG1 responses against rBet v 1 wild-type. The IgG1 antibodies induced by genetically modified rBet v 1 derivatives cross-reacted with natural Bet v 1 and its homologues from alder (Aln g 1) as well as hazel (Cor a 1) and strongly inhibited the binding of birch pollen allergic patients' IgE to Bet v 1 wild-type., Conclusion: Genetically modified hypoallergenic rBet v 1 derivatives induce blocking antibodies in vivo. Their safety and efficacy for the treatment of birch pollen and associated plant allergies can now be evaluated in clinical immunotherapy studies.

Published

2004

2. Mechanisms of immunotherapy with allergoids: lessons for the development of recombinant allergens with reduced IgE-binding activity.

Author

Cromwell O, Kahlert H, Schramm G, Suck R, Nandy A, Weber B, and Fiebig H

Subjects

Allergens therapeutic use, Humans, Recombinant Proteins genetics, Recombinant Proteins immunology, Recombinant Proteins therapeutic use, Allergens genetics, Allergens immunology, Genetic Variation immunology, Immunoglobulin E immunology, Immunotherapy methods

Published

2003

3. Vaccination with Genetically Engineered Allergens Prevents Progression of Allergic Disease

Author

Niederberger, V., Horak, F., Vrtala, S., Spitzauer, S., Valent, P., Reisinger, J., Pelzmann, M., Hayek, B., Kronqvist, M., Gafvelin, G., Grönlund, H., Purohit, A., Suck, R., Fiebig, H., Cromwell, O., Pauli, G., van Hage-Hamsten, M., and Valenta, R.

Published

2004

4. Clinical effects of immunotherapy with genetically modified recombinant birch pollen Bet v 1 derivatives.

Author

Purohit, A., Niederberger, V., Kronqvist, M., Horak, F., Grönneberg, R., Suck, R., Weber, B., Fiebig, H., van Hage, M., Pauli, G., Valenta, R., and Cromwell, O.

Subjects

POLLEN, BIRCH, ALLERGIC rhinitis, CONJUNCTIVITIS, ASTHMA, PLACEBOS, ALLERGENS, IMMUNOTHERAPY

Abstract

Background Birch pollen and pollen from related trees of the Fagales order are a major cause of allergic rhinitis, conjunctivitis, and asthma through the spring season in northern and central Europe. Objective To investigate the clinical effects of injection immunotherapy with genetically modified derivatives of major birch pollen allergen Bet v 1 on pollen-induced allergic symptoms. Methods A three-arm double-blind placebo-controlled immunotherapy study was conducted with one pre-seasonal course of treatment using two derivatives of Bet v 1, namely a recombinant Bet v 1 trimer and an equimolar mixture of two recombinant Bet v 1 fragments together representing the whole protein sequence. Analysis of local and systemic adverse events was performed for 124 patients who had received at least one dose of medication. Clinical efficacy was monitored by symptom medication scores and interval scoring in the per protocol-treated population ( n=84). In addition, skin and nasal provocation responses and allergen-specific antibodies were assessed. Results There were trends towards improvement in the subjects' well-being and clinical symptoms (nasal scores), although comparisons with a placebo group did not show statistical significance in the main end-point, the combined symptom medication score. Reductions in skin and nasal sensitivity were observed for some subjects with a trend for the Bet v 1 trimer to be more effective than the fragments. Treatment induced strong IgG1 and IgG4 allergen-specific antibody responses. Local injection-site reactions were most frequent in the trimer group affecting 59.5% of patients as opposed to 37.8% and 30.6% in the fragment and placebo groups, respectively. Systemic reactions were elicited more frequently by fragments. A large proportion of adverse side-effects appeared hours following injections, and might be attributable to concurrent exposure to related pollens. Conclusion Single courses of injection immunotherapy with Bet v 1 allergen derivatives showed trends towards improved well-being and reduced reactivity to specific allergen provocation, but did not yield significant improvement in the combined symptom medication score in this study. [ABSTRACT FROM AUTHOR]

Published

2008

5. Different allergenic activity of grass pollen allergens revealed by skin testing.

Author

Westritschnig, K., Horak, F., Swoboda, I., Balic, N., Spitzauer, S., Kundi, M., Fiebig, H., Suck, R., Cromwell, O., and Valenta, R.

Subjects

SKIN tests, ALLERGENS, IMMUNOTHERAPY, IMMUNOCHEMISTRY, PATHOLOGICAL physiology, ANTIGENS

Abstract

Background Grass pollen is one of the most important allergen sources. The aim of this study was to compare the in vivo allergenic activity of two recently characterized major grass pollen allergens, Phl p 4 and Phl p 13, with three established major grass pollen allergens, Phl p 1, Phl p 2 and Phl p 5 as a basis for the formulation of a grass pollen allergy vaccine based on purified allergens. Material and methods Eighty-two grass pollen allergic patients were skin prick tested with serial dilutions of approximately equimolar concentrations of the purified allergens in a double-blind study. Results Phl p 4 and Phl p 13 were identified as major grass pollen allergens according to IgE binding frequency (Phl p 4: 85%; Phl p 13: 56%), but exhibited a five to nine-fold lower allergenic skin reactivity compared to Phl p 1, Phl p 2 or Phl p 5. Conclusion Our results indicate that Phl p 4 and Phl p 13 are not essential components for a therapeutic grass pollen vaccine and underpin the importance of evaluating the in vivo allergenic activity of individual allergens for the formulation of therapeutic vaccines based on purified allergens. [ABSTRACT FROM AUTHOR]

Published

2008

6. Characterization of a Hypoallergenic Recombinant Bet v 1 Variant as a Candidate for Allergen-Specific Immunotherapy.

Author

Kahlert, H., Suck, R., Weber, B., Nandy, A., Wald, M., Keller, W., Cromwell, O., and Fiebig, H.

Subjects

ALLERGENS, IMMUNOTHERAPY, CHROMATOGRAPHIC analysis, T cells, CLINICAL immunology, POLLEN

Abstract

Background: Recombinant allergens and especially their hypoallergenic variants are promising candidates for a more effective and safer specific immunotherapy. Methods: Physicochemical and immunological characteristics of a folding variant of recombinant Bet v 1 (rBet v 1-FV) were investigated in comparison to natural Bet v 1 (nBet v 1) and the correctly folded recombinant Bet v 1 (rBet v 1-WT) by SDS-PAGE, size exclusion chromatography, multi-angle light scattering, circular dichroism, immunoblotting and enzyme allergosorbent test inhibition assay for detection of IgE reactivity and ELISA with Bet v 1-specific monoclonal antibodies. The functional IgE reactivity of the different Bet v 1 proteins was investigated using basophil activation in terms of CD203c expression and histamine release. T cell reactivity was investigated using T cell lines raised from birch pollen-allergic subjects against nBet v 1. Immunogenicity was investigated in mice. Results: Physicochemical characterization revealed purity, homogeneity and monomeric properties of rBet v 1-FV. Unlike nBet v 1 and rBet v 1-WT, rBet v 1-FV showed almost no IgE binding in immunoblots. The reduction of allergenicity was further proved by IgE-binding inhibition assays, basophil activation and histamine release. T cell reactivity was completely conserved, as demonstrated by proliferation of Bet v 1-specific T cell lines with multiple epitope specificities. rBet v 1-FV showed strong immunogenicity in mice. Conclusions: Due to its reduced IgE reactivity and decreased capacity to activate basophils, but retained T cell reactivity and strong immunogenicity, rBet v 1-FV proved to be a very promising candidate for specific immunotherapy in birch pollen-allergic subjects. Copyright © 2007 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2008

7. Measurement of basophil-activating capacity of grass pollen allergens, allergoids and hypoallergenic recombinant derivatives by flow cytometry using anti-CD203c.

Author

Kahlert, H., Cromwell, O., and Fiebig, H.

Subjects

BASOPHILS, IMMUNOTHERAPY

Abstract

Summary Background The assessment of the basophil-activating potential is an important aspect in the development of improved preparations for specific immunotherapy. The aim of the study was to evaluate the suitability of CD203c expression as a measure of basophil activation to compare allergoids with original allergen extracts, and recombinant hypoallergenic allergen derivatives with recombinant wild-type and natural allergens. Methods Heparinized whole blood samples from grass pollen allergic subjects were stimulated with grass pollen allergens and allergen derivatives followed by labelling of the basophils with PE-conjugated anti-CD203c. After lysis of the erythrocytes and fixation, the basophils were detected by flow cytometry. In some experiments, histamine release was determined simultaneously. Results Grass pollen allergoids revealed a 10–10 000-fold reduction of basophil-activating capacity measured by CD203c expression. The deletion mutant DM4 of rPhl p 5b showed stronger hypoallergenic characteristics in a range of 50–10 000-fold reduction, whereas a combination mutant of rPhl p 5b and Phl p 6 revealed less hypoallergenic features. Histamine release experiments led to a similar outcome as CD203c measurement. Conclusions The measurement of CD203c expression on basophils by flow cytometry provides a rapid and sensitive method for the estimation of the allergic or hypoallergenic features of allergen preparations. The results demonstrated the hypoallergenicity of grass pollen allergoids and of the rPhl p 5b variant DM4, which may be a candidate in future preparations for specific immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2003

8. Variants of allergen Phlp 5b and reduction of anaphylactogenic potential

Author

Schramm, G., Kahlert, H., Suck, R., Weber, B., Stüwe, H.-T., Müller, W.-D., Bufe, A., Becker, W.-M., Lepp, U., Schlaak, M.-W., Jäger, L., Cromwell, O., and Fiebig, H.

Subjects

*ALLERGENS, *T cells, *POLLEN, *IMMUNOTHERAPY

Abstract

One new approach to improved immunotherapy for type 1 allergy might be the use of modified allergens with reduced IgE reactivity but retained T cell reactivity. By site- directed mutagenesis outside the dominant T cell epitopes, we generated deletion mutants of the grass pollen allergen Phl p 5b. Some of these variants revealed significantly reduced IgE reactivity and histamine releasing capacity compared to the wild-type allergen. Furthermore, in vivo skin prick tests showed that the variants had up to 100 fold lower potency to induce cutaneous reactions than the wild-type allergen. On the other hand, T cell clones and T cell lines from grass pollen-allergic patients showed comparable proliferation after stimulation with these variants and wild-type allergen. Thus, variants of the allergen Phl p 5b with reduced anaphylactogenic potential but retained T cell reactivity could be valuable tools for improved allergen-specific immunotherapy. [Copyright &y& Elsevier]

Published

2003