AI Article Synopsis
- Hom s 2 is an autoantigen linked to IgE autoantibodies in atopic dermatitis, showing similar reactivity to allergens but not causing basophil degranulation.
- Compared to typical allergens, rHom s 2 notably stimulates the release of IFN-gamma from immune cells in both atopic and non-atopic individuals.
- The IFN-gamma produced can lead to damage in respiratory and skin cells, a process that can be blocked by anti-IFN-gamma antibodies.
Article Abstract
Hom s 2, the alpha-chain of the nascent polypeptide-associated complex, is an intracellular autoantigen that has been identified with IgE autoantibodies from atopic dermatitis patients. We investigated the humoral and cellular immune response to purified recombinant Hom s 2 (rHom s 2). rHom s 2 exhibited IgE reactivity comparable to exogenous allergens, but did not induce relevant basophil cell degranulation. The latter may be attributed to the fact that patients recognized single epitopes on Hom s 2 as revealed by IgE epitope mapping with rHom s 2 fragments. In contrast to exogenous allergens, rHom s 2 had the intrinsic ability to induce the release of IFN-gamma in cultured peripheral blood mononuclear cells from atopic as well as non-atopic individuals. IFN-gamma-containing culture supernatants from Hom s 2-stimulated peripheral blood mononuclear cells caused disintegration of respiratory epithelial cell layers and apoptosis of skin keratinocytes, which could be inhibited with a neutralizing anti-IFN-gamma antibody. Our data demonstrate that the Hom s 2 autoantigen can cause IFN-gamma-mediated cell damage.
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| http://dx.doi.org/10.1038/sj.jid.5701195 | DOI Listing |
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