Your search keyword '"Rhyner Claudio"' showing total 8 results

1. State‐of‐the‐art in marketed adjuvants and formulations in Allergen Immunotherapy: A position paper of the European Academy of Allergy and Clinical Immunology (EAACI).

Author

Jensen‐Jarolim, Erika, Bachmann, Martin F., Bonini, Sergio, Jacobsen, Lars, Jutel, Marek, Klimek, Ludger, Mahler, Vera, Mösges, Ralph, Moingeon, Philippe, O´Hehir, Robyn E., Palomares, Oscar, Pfaar, Oliver, Renz, Harald, Rhyner, Claudio, Roth‐Walter, Franziska, Rudenko, Michael, Savolainen, Johannes, Schmidt‐Weber, Carsten B., Traidl‐Hoffmann, Claudia, and Kündig, Thomas

Subjects

CLINICAL immunology, ALLERGENS, ALLERGIES, IMMUNOTHERAPY, PATIENT compliance

Abstract

Since the introduction of allergen immunotherapy (AIT) over 100 years ago, focus has been on standardization of allergen extracts, with reliable molecular composition of allergens receiving the highest attention. While adjuvants play a major role in European AIT, they have been less well studied. In this Position Paper, we summarize current unmet needs of adjuvants in AIT citing current evidence. Four adjuvants are used in products marketed in Europe: aluminium hydroxide (Al(OH)3) is the most frequently used adjuvant, with microcrystalline tyrosine (MCT), monophosphoryl lipid A (MPLA) and calcium phosphate (CaP) used less frequently. Recent studies on humans, and using mouse models, have characterized in part the mechanisms of action of adjuvants on pre‐existing immune responses. AIT differs from prophylactic vaccines that provoke immunity to infectious agents, as in allergy the patient is presensitized to the antigen. The intended mode of action of adjuvants is to simultaneously enhance the immunogenicity of the allergen, while precipitating the allergen at the injection site to reduce the risk of anaphylaxis. Contrasting immune effects are seen with different adjuvants. Aluminium hydroxide initially boosts Th2 responses, while the other adjuvants utilized in AIT redirect the Th2 immune response towards Th1 immunity. After varying lengths of time, each of the adjuvants supports tolerance. Further studies of the mechanisms of action of adjuvants may advise shorter treatment periods than the current three‐to‐five‐year regimens, enhancing patient adherence. Improved lead compounds from the adjuvant pipeline are under development and are explored for their capacity to fill this unmet need. [ABSTRACT FROM AUTHOR]

Published

2020

2. EAACI position paper: Comparing insect hypersensitivity induced by bite, sting, inhalation or ingestion in human beings and animals.

Author

Pali‐Schöll, Isabella, Blank, Simon, Verhoeckx, Kitty, Mueller, Ralf S., Janda, Jozef, Marti, Eliane, Seida, Ahmed A., Rhyner, Claudio, DeBoer, Douglas J., and Jensen‐Jarolim, Erika

Subjects

HUMAN beings, INSECT bites & stings, INGESTION, INSECTS, ALLERGIES, SYMPTOMS

Abstract

Adverse reactions to insects occur in both human and veterinary patients. Systematic comparison may lead to improved recommendations for prevention and treatment in all species. In this position paper, we summarize the current knowledge on insect allergy induced via stings, bites, inhalation or ingestion, and compare reactions in companion animals to those in people. With few exceptions, the situation in human insect allergy is better documented than in animals. We focus on a review of recent literature and give overviews of the epidemiology and clinical signs. We discuss allergen sources and allergenic molecules to the extent described, and aspects of diagnosis, prophylaxis, management and therapy. [ABSTRACT FROM AUTHOR]

Published

2019

3. Longitudinal analysis of allergen‐specific IgE and IgG subclasses as potential predictors of insect bite hypersensitivity following first exposure to <italic>Culicoides</italic> in Icelandic horses.

Author

Ziegler, Anja, Hamza, Eman, Jonsdottir, Sigridur, Rhyner, Claudio, Wagner, Bettina, Schüpbach, Gertraud, Svansson, Vilhjalmur, Torsteinsdottir, Sigurbjorg, and Marti, Eliane

Subjects

IMMUNOGLOBULIN E, BITES & stings, IMMUNOGLOBULINS, ALLERGIES, IMMUNOLOGIC diseases

Abstract

Copyright of Veterinary Dermatology is the property of Wiley-Blackwell and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2018

4. In Vitro Evolution of Allergy Vaccine Candidates, with Maintained Structure, but Reduced B Cell and T Cell Activation Capacity.

Author

Nilsson, Ola B., Adedoyin, Justus, Rhyner, Claudio, Neimert-Andersson, Theresa, Grundström, Jeanette, Berndt, Kurt D., Crameri, Reto, and Grönlund, Hans

Subjects

ALLERGIES, IMMUNOGLOBULIN E, INFLAMMATION, IMMUNOTHERAPY, T cells, ASTHMA, B cells, SYMPTOMS, VACCINATION

Abstract

Allergy and asthma to cat (Felis domesticus) affects about 10% of the population in affluent countries. Immediate allergic symptoms are primarily mediated via IgE antibodies binding to B cell epitopes, whereas late phase inflammatory reactions are mediated via activated T cell recognition of allergen-specific T cell epitopes. Allergen-specific immunotherapy relieves symptoms and is the only treatment inducing a long-lasting protection by induction of protective immune responses. The aim of this study was to produce an allergy vaccine designed with the combined features of attenuated T cell activation, reduced anaphylactic properties, retained molecular integrity and induction of efficient IgE blocking IgG antibodies for safer and efficacious treatment of patients with allergy and asthma to cat. The template gene coding for rFel d 1 was used to introduce random mutations, which was subsequently expressed in large phage libraries. Despite accumulated mutations by up to 7 rounds of iterative error-prone PCR and biopanning, surface topology and structure was essentially maintained using IgE-antibodies from cat allergic patients for phage enrichment. Four candidates were isolated, displaying similar or lower IgE binding, reduced anaphylactic activity as measured by their capacity to induce basophil degranulation and, importantly, a significantly lower T cell reactivity in lymphoproliferative assays compared to the original rFel d 1. In addition, all mutants showed ability to induce blocking antibodies in immunized mice.The approach presented here provides a straightforward procedure to generate a novel type of allergy vaccines for safer and efficacious treatment of allergic patients. [ABSTRACT FROM AUTHOR]

Published

2011

5. Cross-reactivity among fungal allergens: a clinically relevant phenomenon?

Author

Crameri, Reto, Zeller, Sabine, Glaser, Andreas G., Vilhelmsson, Monica, and Rhyner, Claudio

Subjects

FUNGI, TRANSFER factor (Immunology), ALLERGIES, MOLECULAR cloning, ALLERGENS

Abstract

Atopic patients suffering from allergic asthma, allergic rhinitis, or atopic eczema often have detectable levels of serum IgE antibodies to fungi. Although the association between fungal sensitisation and different forms of allergic diseases, including allergic asthma and life-threatening allergic bronchopulmonary aspergillosis, is well established, the clinical relevance of cross-reactivity among different fungal species remains largely unknown. Recent progress in molecular cloning of fungal allergens and the availability of more than 40 completely sequenced fungal genomes facilitates characterisation, cloning, and production of highly pure recombinant allergens, identification of homologous and orthologous allergens widespread among the fungal kingdom, in silico prediction, and experimental in vitro and in vivo verification of cross-reactivity between homologous pan-allergens. These studies indicate that cross-reactivity is an important component of fungal sensitisation. [ABSTRACT FROM AUTHOR]

Published

2009

6. A major allergen gene-fusion protein for potential usage in allergen-specific immunotherapy.

Author

Kussebi, Fatimah, Karamloo, Fariba, Rhyner, Claudio, Schmid-Grendelmeier, Peter, Salagianni, Maria, Mannhart, Christian, Akdis, Mübeccel, Soldatova, Lyudmilla, Markovic-Housley, Zora, von Beust, Barbara R., Kündig, Thomas, Kemeny, David M., Blaser, Kurt, Crameri, Reto, and Akdis, Cezmi A.

Subjects

ALLERGENS, IMMUNOTHERAPY, ALLERGIES, IMMUNOLOGIC diseases, BEE venom, ANAPHYLAXIS, T cells, IMMUNIZATION, VACCINATION, THERAPEUTICS

Abstract

Background: Specific immunotherapy is a common treatment of allergic diseases and could potentially be applied to other immunologic disorders. Despite its use in clinical practice, more defined and safer allergy vaccine preparations are required. Differences between epitopes of IgE that recognize the 3-dimensional structure of allergens and T cells that recognize linear amino acid sequences provide a suitable tool for novel vaccine development for specific immunotherapy. Objective: The aim of the study was to delete B-cell epitopes and prevent IgE crosslinking, but to preserve T-cell epitopes by fusion of 2 major allergens of bee venom because of a change in the conformation. Methods: By genetic engineering, we produced a fusion protein composed of the 2 major bee venom allergens: phospholipase A2 (Api m 1) and hyaluronidase (Api m 2). Results: The Api m [1/2] fusion protein induced T-cell proliferation and both TH1-type and TH2-type cytokine responses. In contrast, IgE reactivity was abolished, and profoundly reduced basophil degranulation and type 1 skin test reactivity was observed. Pretreatment of mice with Api m [1/2] fusion protein significantly suppressed the development of specific IgE as well as other antibody isotypes after immunization with the native allergen. Conclusion: The novel fusion protein of 2 major allergens bypasses IgE binding and mast cell/basophil IgE FcεRI crosslinking and protects from IgE development. [ABSTRACT FROM AUTHOR]

Published

2005

7. A preventive immunization approach against insect bite hypersensitivity: Intralymphatic injection with recombinant allergens in Alum or Alum and monophosphoryl lipid A.

Author

Jonsdottir, Sigridur, Svansson, Vilhjalmur, Stefansdottir, Sara Bjork, Schüpbach, Gertraud, Rhyner, Claudio, Marti, Eliane, and Torsteinsdottir, Sigurbjorg

Subjects

*ALLERGIES, *INSECT bites & stings, *ALUM, *IMMUNOGLOBULIN E, *CULICOIDES, *ETIOLOGY of diseases, *IMMUNOLOGICAL adjuvants

Abstract

Insect bite hypersensitivity (IBH) is an IgE-mediated dermatitis of horses caused by bites of Culicoides insects, not indigenous to Iceland. Horses born in Iceland and exported to Culicoides -rich areas are frequently affected with IBH. The aims of the study were to compare immunization with recombinant allergens using the adjuvant aluminum hydroxide (Alum) alone or combined with monophosphoryl lipid A (MPLA) for development of a preventive immunization against IBH. Twelve healthy Icelandic horses were vaccinated intralymphatically three times with 10 μg each of four recombinant Culicoides nubeculosus allergens in Alum or in Alum/MPLA. Injection with allergens in both Alum and Alum/MPLA resulted in significant increase in specific IgG subclasses and IgA against all r-allergens with no significant differences between the adjuvant groups. The induced antibodies from both groups could block binding of allergen specific IgE from IBH affected horses to a similar extent. No IgE-mediated reactions were induced. Allergen-stimulated PBMC from Alum/MPLA horses but not from Alum only horses produced significantly more IFNγ and IL-10 than PBMC from non-vaccinated control horses. In conclusion, intralymphatic administration of small amounts of pure allergens in Alum/MPLA induces high IgG antibody levels and Th1/Treg immune response and is a promising approach for immunoprophylaxis and immunotherapy against IBH. [ABSTRACT FROM AUTHOR]

Published

2016

8. Developing a preventive immunization approach against insect bite hypersensitivity using recombinant allergens: A pilot study.

Author

Jonsdottir, Sigridur, Hamza, Eman, Janda, Jozef, Rhyner, Claudio, Meinke, Andreas, Marti, Eliane, Svansson, Vilhjalmur, and Torsteinsdottir, Sigurbjorg

Subjects

*INSECT bites & stings, *IMMUNIZATION, *ALLERGIES, *CONTACT dermatitis, *RECOMBINANT molecules, *PILOT projects, *PREVENTION

Abstract

Insect bite hypersensitivity (IBH) is an allergic dermatitis of horses caused by bites of midges ( Culicoides spp.). IgE-mediated reactions are often involved in the pathogenesis of this disease. IBH does not occur in Iceland due to the absence of Culicoides , but it occurs with a high frequency in Icelandic horses exported to mainland Europe, where Culicoides are present. We hypothesize that immunization with the Culicoides allergens before export could reduce the incidence of IBH in exported Icelandic horses. The aim of the present study was therefore to compare intradermal and intralymphatic vaccination using four purified recombinant allergens, in combination with a Th1 focusing adjuvant. Twelve horses were vaccinated three times with 10 μg of each of the four recombinant Culicoides nubeculosus allergens. Six horses were injected intralymphatically, three with and three without IC31 ® , and six were injected intradermally, in the presence or absence of IC31 ® . Antibody responses were measured by immunoblots and ELISA, potential sensitization in a sulfidoleukotriene release test and an intradermal test, cytokine and FoxP3 expression with real time PCR following in vitro stimulation of PBMC. Immunization with the r-allergens induced a significant increase in levels of r-allergen-specific IgG1, IgG1/3, IgG4/7, IgG5 and IgG(T). Application of the r-allergens in IC31 ® adjuvant resulted in a significantly higher IgG1, IgG1/3, IgG4/7 allergen-specific response. Intralymphatic injection was slightly more efficient than intradermal injection, but the difference did not reach significance. Testing of the blocking activity of the sera from the horses immunized intralymphatically with IC31 ® showed that the generated IgG antibodies were able to partly block binding of serum IgE from an IBH-affected horse to these r-allergens. Furthermore, IgG antibodies bound to protein bands on blots of C. nubeculosus salivary gland extract. No allergen-specific IgE was induced and there was no indication of induction of IgE-mediated reactions, as horses neither responded to Culicoides extract stimulation in a sulfidoleukotriene release test, nor developed a relevant immediate hypersensitivity reaction to the recombinant allergens in skin test. IL-4 expression was significantly higher in horses vaccinated intralymphatically without IC31 ® , as compared to horses intradermally vaccinated with IC31 ® . Both routes gave higher IL-10 expression with IC31 ® . Both intralymphatic and intradermal vaccination of horses with recombinant allergens in IC31 ® adjuvant induced an immune response without adverse effects and without IgE production. The horses were not sensitized and produced IgG that could inhibit allergen-specific IgE binding. We therefore conclude that both the injection routes and the IC31 ® adjuvant are strong candidates for further development of immunoprophylaxis and therapy in horses. [ABSTRACT FROM AUTHOR]

Published

2015