Literature DB >> 20584008

Early markers for protective mechanisms during rush venom immunotherapy.

C Bussmann1, J Xia, J-P Allam, L Maintz, T Bieber, N Novak.   

Abstract

BACKGROUND: Allergen-specific venom immunotherapy (VIT) represents the only rational-based option to treat allergic sensitizations against bee and wasp venom. So far, there is not much knowledge about early induction of protective and tolerogenic pathways during VIT.
OBJECTIVES: To identify the earliest markers for protective mechanisms against allergic reactions in the peripheral blood during the build-up phase of VIT.
METHODS: PBMC and monocytes were isolated, and serum samples were taken before and during a five day build-up phase from 65 hymenoptera venom allergic patients. Expression level of tolerogenic markers was analyzed on mRNA and protein level. Serum levels of different soluble tolerogenic factors were measured.
RESULTS: We observed significantly enhanced tryptophan degradation, elevated ILT4 expression of monocytes as well as IL-10 production of CD3(+) T cells only a few hours after the first injection on day 1, followed by increased IL-10 serum levels, monocyte apoptosis and elevated intracellular cAMP levels of monocytes on day 3 combined with a higher ILT3 protein expression and IL-10 secretion of monocytes on day 5.
CONCLUSION: From these data, we conclude that tryptophan depletion, ILT3/4-mediated inhibition, higher IL-10 production as well as intracellular cAMP might contribute to early induction of protective mechanisms against allergic reactions during the build-up phase of VIT.
© 2010 John Wiley & Sons A/S.

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Year:  2010        PMID: 20584008     DOI: 10.1111/j.1398-9995.2010.02430.x

Source DB:  PubMed          Journal:  Allergy        ISSN: 0105-4538            Impact factor:   13.146


  18 in total

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