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1. T cells specific to multiple Bet v 1 peptides are highly cross-reactive toward the corresponding peptides from the homologous group of tree pollens.

2. The role of allergen-specific IgE, IgG and IgA in allergic disease.

3. Autologous enzyme-linked immunosorbent facilitated antigen binding detects IgE-blocking activity based on direct competition between allergen-specific IgE and non-IgE.

4. Differential induction of allergen-specific IgA responses following timothy grass subcutaneous and sublingual immunotherapy.

5. Treatment Effect of the Tree Pollen SLIT-Tablet on Allergic Rhinoconjunctivitis During Oak Pollen Season.

6. Basophil sensitivity reflects long-term clinical outcome of subcutaneous immunotherapy in grass pollen-allergic patients.

7. Simplified AIT for allergy to several tree pollens-Arguments from the immune outcome analyses following treatment with SQ tree SLIT-tablet.

8. Allergy to oak pollen in North America.

9. The IgE Blocking Activity Induced by Dermatophagoides pteronyssinus Subcutaneous Immunotherapy Does Not Correlate with Specific IgA but with IgG4 in both Serum and Saliva.

10. Diverse and highly cross-reactive T-cell responses in ragweed allergic patients independent of geographical region.

11. Legends of allergy and immunology: Henning Løwenstein.

12. Persistent regulatory T-cell response 2 years after 3 years of grass tablet SLIT: Links to reduced eosinophil counts, sIgE levels, and clinical benefit.

13. A birch sublingual allergy immunotherapy tablet reduces rhinoconjunctivitis symptoms when exposed to birch and oak and induces IgG 4 to allergens from all trees in the birch homologous group.

14. Genetically engineered cell factories produce glycoengineered vaccines that target antigen-presenting cells and reduce antigen-specific T-cell reactivity.

15. Strong and frequent T-cell responses to the minor allergen Phl p 12 in Spanish patients IgE-sensitized to Profilins.

17. Immunoproteomic analysis of house dust mite antigens reveals distinct classes of dominant T cell antigens according to function and serological reactivity.

18. Distinct modulation of allergic T cell responses by subcutaneous vs. sublingual allergen-specific immunotherapy.

19. Pretreatment IgE sensitization patterns determine the molecular profile of the IgG4 response during updosing of subcutaneous immunotherapy with timothy grass pollen extract.

20. Grass pollen immunotherapy: where are we now.

21. Polarized Airway Epithelial Models for Immunological Co-Culture Studies.

22. Effect of Polarization on Airway Epithelial Conditioning of Monocyte-Derived Dendritic Cells.

23. Airway responses towards allergens - from the airway epithelium to T cells.

24. Direct contact between dendritic cells and bronchial epithelial cells inhibits T cell recall responses towards mite and pollen allergen extracts in vitro.

25. Early improvement in basophil sensitivity predicts symptom relief with grass pollen immunotherapy.

26. Immunological comparison of allergen immunotherapy tablet treatment and subcutaneous immunotherapy against grass allergy.

27. Cell-free detection of allergen-IgE cross-linking with immobilized phase CD23: inhibition by blocking antibody responses after immunotherapy.

29. Human leukocyte antigen-G and regulatory T cells during specific immunotherapy for pollen allergy.

30. Birch pollen immunotherapy results in long-term loss of Bet v 1-specific TH2 responses, transient TR1 activation, and synthesis of IgE-blocking antibodies.

31. Antibody repertoire complexity and effector cell biology determined by assays for IgE-mediated basophil and T-cell activation.

32. The complexity of allergic patients' IgE repertoire correlates with serum concentration of allergen-specific IgE.

33. Reduced in vitro T-cell responses induced by glutaraldehyde-modified allergen extracts are caused mainly by retarded internalization of dendritic cells.

34. Functional rather than immunoreactive levels of IgG4 correlate closely with clinical response to grass pollen immunotherapy.

35. Epitope grafting, re-creating a conformational Bet v 1 antibody epitope on the surface of the homologous apple allergen Mal d 1.

36. Facilitated antigen presentation and its inhibition by blocking IgG antibodies depends on IgE repertoire complexity.

37. Phl p 5 resorption in human oral mucosa leads to dose-dependent and time-dependent allergen binding by oral mucosal Langerhans cells, attenuates their maturation, and enhances their migratory and TGF-beta1 and IL-10-producing properties.

38. The T cell response to major grass allergens is regulated and includes IL-10 production in atopic but not in non-atopic subjects.

39. Allergenicity, immunogenicity and dose-relationship of three intact allergen vaccines and four allergoid vaccines for subcutaneous grass pollen immunotherapy.

40. A double-blind placebo-controlled birch allergy vaccination study II: correlation between inhibition of IgE binding, histamine release and facilitated allergen presentation.

41. Comparison of allergenicity and immunogenicity of an intact allergen vaccine and commercially available allergoid products for birch pollen immunotherapy.

42. Chemical modification of birch allergen extract leads to a reduction in allergenicity as well as immunogenicity.

43. IgE-mediated allergen presentation and blocking antibodies: regulation of T-cell activation in allergy.

44. Allergy vaccine engineering: epitope modulation of recombinant Bet v 1 reduces IgE binding but retains protein folding pattern for induction of protective blocking-antibody responses.

45. A double-blind, placebo-controlled birch allergy vaccination study: inhibition of CD23-mediated serum-immunoglobulin E-facilitated allergen presentation.

46. IL-15 induces unspecific effector functions in human peptide-specific CD8+ T-cell cultures.

47. A HLA-A2 restricted human CTL line recognizes a novel tumor cell expressed p53 epitope.

48. Specific killing of P53 mutated tumor cell lines by a cross-reactive human HLA-A2-restricted P53-specific CTL line.

49. Grass allergen-specific T-cells of atopic patients.

50. Maturation of dendritic cells by recombinant human CD40L-trimer leads to a homogeneous cell population with enhanced surface marker expression and increased cytokine production.

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