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Department of Internal Medicine, Immunoallergology and Respiratory Disease Unit, University of Florence, Florence, Italy
DNA vaccination is an effective approach in inducing the switch of
murine immune responses from a Th2 to a Th1 profile of cytokine
production that has been related to the activity of unmethylated CpG
motifs present in bacterial, but not mammalian, DNA. We report here
that some synthetic phosphorothioate, but not phosphodiester,
oligodeoxynucleotides (ODNs) were able to induce B cell proliferation
and to shift the in vitro differentiation of Dermatophagoides
pteronyssinus group 1-specific human CD4+ T cells
from atopic donors into Th cell effectors showing a prevalent Th1,
instead of Th2, cytokine profile. This latter effect was completely
blocked by the neutralization of IL-12 and IFN (
and
) in bulk
culture, suggesting that the Th1-inducing activity of phosphorothioate
ODNs was mediated by their ability to stimulate the production of these
cytokines by monocytes, dendritic, and NK cells. Cytosine methylation
abolished the Th1-inducing activity of ODNs; however, CpG
dinucleotide-containing ODNs exhibited the Th1-shifting effect
independently of the presence or the absence of CpG motifs
(5'-pur-pur-CpG-pyr-pyr-3'). Moreover, the inversion of CpG to GpC
resulted only in a partial reduction of this activity, suggesting that
the motif responsible for the Th1-skewing effect in humans is at least
partially different from that previously defined in mice. These results
support the concept that the injection of allergens mixed to, or
conjugated with, appropriate ODNs may provide a novel allergen-specific
immunotherapeutic regimen for the treatment of allergic
disorders.
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