Development and preliminary clinical evaluation of a peptide immunotherapy vaccine for cat allergy - 10/08/11
Reprint requests: Mark Larché, PhD, Canada Research Chair in Allergy & Immune Tolerance, McMaster University/GSK Chair in Lung Immunology; Divisions of Clinical Immunology and Allergy and Respirology, Department of Medicine, McMaster University, Firestone Institute for Respiratory Health, T2131-1, 2nd Floor, Juravinski Tower, St Joseph’s Hospital Healthcare, 50 Charlton Ave East, Hamilton, Ontario L8N 4A6, Canada.Abstract |
Background |
Allergic sensitization to cat allergens is common and represents a major risk factor for asthma. Specific immunotherapy (SIT) is effective but cumbersome and associated with IgE-dependent adverse events. Immunotherapy targeting allergen-specific T cells, with synthetic peptides representing T-cell epitopes, might improve safety and reduce the duration of treatment.
Objective |
We sought to define major T-cell epitopes of Fel d 1 for peptide immunotherapy, generate a peptide vaccine, and evaluate its safety and tolerability in subjects with cat allergy.
Methods |
We determined the binding affinities of Fel d 1 peptides for 10 commonly expressed HLA-DR molecules. Functionally immunodominant peptides were identified by means of proliferation and cytokine secretion. Histamine-releasing activity was assessed, and a peptide vaccine was formulated. Safety and tolerability were evaluated in a dose-ranging phase IIa clinical trial.
Results |
MHC-binding sequences were identified throughout Fel d 1. Some regions contained multiple overlapping T-cell epitopes that bound multiple MHC molecules. Immunodominant sequences were identified on the basis of proliferative and cytokine (IFN-γ, IL-10, and IL-13) responses. Cat allergen extract, but not peptides, induced histamine release in blood basophils. A single administration of peptide vaccine was safe and well tolerated. The dose of vaccine resulting in the greatest inhibition of the late-phase skin response to intradermal whole allergen challenge was 3 nmol.
Conclusions |
Fel d 1 contains multiple overlapping MHC-binding motifs. A peptide vaccine comprising the immunodominant regions of the allergen was safe and well tolerated when given to subjects with cat allergy as a single dose. The dose of vaccine resulting in the greatest reduction in late-phase skin response was defined for future clinical development.
Le texte complet de cet article est disponible en PDF.Key words : Immunotherapy, allergy, T cell, epitope, peptide, MHC, immune tolerance, vaccine
Abbreviations used : AD, EPSR, HEP, LPSR, PPD, SAE, TEAE
Plan
| Supported by Circassia Ltd. |
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| Disclosure of potential conflict of interest: R. P. Hafner and P. Laidler are employees of Circassia Ltd. A. B. Kay is a founder, stockholder, and consultant for Circassia Ltd. M. Larché is founder, stockholder, and consultant of Circassia Ltd and a founding scientist of Adiga Life Sciences and has received research support from both companies. The rest of the authors have declared that they have no conflict of interest. |
Vol 127 - N° 1
P. 89 - janvier 2011 Retour au numéro
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