The enigma of IgE+ B-cell memory in human subjects - 30/03/13
Corresponding author: Rob C. Aalberse, PhD, Department of Immunopathology, Sanquin Blood Supply Foundation, Plesmanlaan 125,1066 CX, Amsterdam, The Netherlands.Abstract |
Our understanding of the origin and fate of the IgE-switched B cell has been markedly improved by studies in mouse models. The immediate precursor of the IgE-switched B cell is either a relatively naive nonswitched B cell or a mature IgG-switched B cell. These 2 routes are referred to as the direct and indirect pathways, respectively. IgE responses derived from each pathway differ significantly, largely reflecting the difference in time spent in a germinal center and thus time for clonal expansion, somatic hypermutation, affinity maturation, and acquisition of a memory phenotype. The clinical and therapeutic implications for IgE responses in human subjects are still a matter of debate, largely because the immunization procedures used in the animal models are significantly different from classical atopic sensitization to allergens from pollen and mites. On the basis of the limited information available, it seems likely that these atopic IgE responses are characterized by a relatively low IgG/IgE ratio, low B-cell memory, and modest affinity maturation, which fits well with the direct switching pathway. It is still unresolved how the IgE response evolves to cover a wide epitope repertoire involving many epitopes per allergen, as well as many different allergens from a single allergen source.
Le texte complet de cet article est disponible en PDF.Key words : IgE, B cells, IgE+ B cells, memory B cells, plasma cells, allergy, germinal center
Abbreviations used : CDR, GC, PC, SHM, SIT
Plan
| J.M.D. has received honoraria payments for education presentations and contracted research funds from Stallergenes Pty Ltd and is supported by funds from the Australian National Health and Medical Research Council, the Asthma Foundation of Queensland, and the University of Queensland. |
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| Disclosure of potential conflict of interest: J. M. Davies has consultancy arrangements with Stallergenes Pty Ltd, France; is employed by the University of Queensland; has received one or more grants from or has one or more grants pending with the National Health Medical Research Council of Australia, the Asthma Foundation of Queensland, the University of Queensland, and the Australian Society for Clinical Immunology and Allergy; has received one or more payments for lecturing from or is on the speakers’ bureau for Stallergenes Pty Ltd; and has received one or more payments for travel/accommodations/meeting expenses from Stallergenes for delivery of research presentations. T. A. Platts-Mills has received one or more grants from or has one or more grants pending with the National Institutes of Health/National Institute of Allergy and Infectious Diseases. R. C. Aalberse declares that he has no relevant conflicts of interest. |
Vol 131 - N° 4
P. 972-976 - avril 2013 Retour au numéro
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