Recombinant Fusion Allergens, Cry j 1 and Cry j 2 from Japanese Cedar Pollen, Conjugated with Polyethylene Glycol Potentiate the Attenuation of Cry j 1-Specific IgE Production in Cry j 1-Sensitized Mice and Japanese Cedar Pollen Allergen-Sensitized Monkeys

Fujimura, Takashi; Fujinami, Koji; Ishikawa, Ryosuke; Tateno, Minoru; Terada, Yoshio; Okumura, Yasushi; Ohta, Hisashi; Miyazaki, Hiroyuki; Taniguchi, Masaru

doi:10.1159/000441141

Cited by 13 publications

(14 citation statements)

References 23 publications

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“…Promising results have been attained with these carrier molecules, among which are bacteriophage Qb-derived virus-like particles [121], hepatitis B virus pre-S protein [122-124], and polyethylene glycol [125]. …”

Section: Allergen-specific Immunotherapymentioning

confidence: 99%

Ragweed Pollen Allergy: Burden, Characteristics, and Management of an Imported Allergen Source in Europe

Chen

Marusciac

Tamas

et al. 2018

Int Arch Allergy Immunol

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Ambrosia artemisiifolia, also known as common or short ragweed, is an invasive annual flowering herbaceous plant that has its origin in North America. Nowadays, ragweed can be found in many areas worldwide. Ragweed pollen is known for its high potential to cause type I allergic reactions in late summer and autumn and represents a major health problem in America and several countries in Europe. Climate change and urbanization, as well as long distance transport capacity, enhance the spread of ragweed pollen. Therefore ragweed is becoming domestic in non-invaded areas which in turn will increase the sensitization rate. So far 11 ragweed allergens have been described and, according to IgE reactivity, Amb a 1 and Amb a 11 seem to be major allergens. Sensitization rates of the other allergens vary between 10 and 50%. Most of the allergens have already been recombinantly produced, but most of them have not been characterized regarding their allergenic activity, therefore no conclusion on the clinical relevance of all the allergens can be made, which is important and necessary for an accurate diagnosis. Pharmacotherapy is the most common treatment for ragweed pollen allergy but fails to impact on the course of allergy. Allergen-specific immunotherapy (AIT) is the only causative and disease-modifying treatment of allergy with long-lasting effects, but currently it is based on the administration of ragweed pollen extract or Amb a 1 only. In order to improve ragweed pollen AIT, new strategies are required with higher efficacy and safety.

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Section: Allergen-specific Immunotherapymentioning

confidence: 99%

Ragweed Pollen Allergy: Burden, Characteristics, and Management of an Imported Allergen Source in Europe

Chen

Marusciac

Tamas

et al. 2018

Int Arch Allergy Immunol

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“…Karamloo et al [76 ]could show that a hybrid consisting of fragmented sequences of the 3 bee venom major allergens Api m 1, 2, and 3 had preserved T-cell epitopes, had lost the B cell epitopes of all 3 allergens, and possessed a highly reduced IgE cross-linking ability on human mast cells and basophils as well as a strongly reduced skin test reactivity. The 2 major allergens of Japanese cedar ( Cryptomeria japonica ) pollen, Cry j 1 and Cry j 2, were expressed as a fusion protein and then conjugated to polyethylene glycol to improve their solubility and to create a safer vaccine [77]. Treatment of mice and monkeys with this vaccine resulted in a significant increase of Cry j 1-specific IgG.…”

Section: Vaccine Developmentmentioning

confidence: 99%

Recombinant Allergens in Structural Biology, Diagnosis, and Immunotherapy

Tscheppe

Breiteneder²

2017

Int Arch Allergy Immunol

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The years 1988-1995 witnessed the beginning of allergen cloning and the generation of recombinant allergens, which opened up new avenues for the diagnosis and research of human allergic diseases. Most crystal and solution structures of allergens have been obtained using recombinant allergens. Structural information on allergens allows insights into their evolutionary biology, illustrates clinically observed cross-reactivities, and makes the design of hypoallergenic derivatives for allergy vaccines possible. Recombinant allergens are widely used in molecule-based allergy diagnosis such as protein microarrays or suspension arrays. Recombinant technologies have been used to produce well-characterized, noncontaminated vaccine components with known biological activities including a variety of allergen derivatives with reduced IgE reactivity. Such recombinant hypoallergens as well as wild-type recombinant allergens have been used successfully in several immunotherapy trials for more than a decade to treat birch and grass pollen allergy. As a more recent application, the development of antibody repertoires directed against conformational epitopes during immunotherapy has been monitored by recombinant allergen chimeras. Although much progress has been made, the number and quality of recombinant allergens will undoubtedly increase and keep improving our knowledge in basic scientific investigations, diagnosis, and therapy of human allergic diseases.

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“…To break the Cry j 1 and Cry j 2 conformational structures, the majority of cysteine residues were replaced with serine residues. 88 The modified fusion protein was then conjugated with polyethylene glycol (PEG) and used to treat CPE sensitized monkeys. After four weekly subcutaneous injections of the PEG-conjugated fusion protein administered at a 1mg/0.5ml dose, the production of Cry j 1 specific IgG was significantly increased when compared to the baseline prior to treatment and significantly reduced Cry j 1 specific IgE antibody production.…”

Section: Peg Conjugated Recombinant Hypoallergenic Proteinmentioning

confidence: 99%

Next generation immunotherapy for tree pollen allergies

Romeu-Bonilla

Heiland

2017

Human Vaccines & Immunotherapeutics

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Tree pollen induced allergies are one of the major medical and public health burdens in the industrialized world. Allergen-Specific Immunotherapy (AIT) through subcutaneous injection or sublingual delivery is the only approved therapy with curative potential to pollen induced allergies. AIT often is associated with severe side effects and requires long-term treatment. Safer, more effective and convenient allergen specific immunotherapies remain an unmet need. In this review article, we discuss the current progress in applying protein and peptide-based approaches and DNA vaccines to the clinical challenges posed by tree pollen allergies through the lens of preclinical animal models and clinical trials, with an emphasis on the birch and Japanese red cedar pollen induced allergies.

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Recombinant Fusion Allergens, Cry j 1 and Cry j 2 from Japanese Cedar Pollen, Conjugated with Polyethylene Glycol Potentiate the Attenuation of Cry j 1-Specific IgE Production in Cry j 1-Sensitized Mice and Japanese Cedar Pollen Allergen-Sensitized Monkeys

Cited by 13 publications

References 23 publications

Ragweed Pollen Allergy: Burden, Characteristics, and Management of an Imported Allergen Source in Europe

Ragweed Pollen Allergy: Burden, Characteristics, and Management of an Imported Allergen Source in Europe

Recombinant Allergens in Structural Biology, Diagnosis, and Immunotherapy

Next generation immunotherapy for tree pollen allergies

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