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Asthma and Allergic Diseases Center, Department of Internal Medicine, University of Virginia, Charlottesville, VA 22908
Distinct immune responses in humans to the Trichophyton
rubrum Ag, Tri r 2, are associated with different patterns of T
cell epitope recognition based on in vitro proliferation to peptides
derived from this 29-kDa protein. Specifically, the amino-terminal
immunodominant epitope, peptide 5 (P5), stimulates strong T cell
proliferative responses in subjects with delayed (DTH), but not
immediate (IH) hypersensitivity skin tests. Evidence of a role for
cytokines or changes in epitope recognition over time was examined in
responses to Trichophyton using primary PBMC cultures
established from seven IH and seven DTH subjects. Responses stimulated
by Tri r 2 were dominated by the Th1 cytokine IFN-
(IFN-
:IL-5
4:1) in five DTH subjects, even in the presence
of Th2-dominated responses (IFN-
:IL-5
3:1) to a subset of
major epitopes. Paradoxically, P5 induced IL-5 and IL-10 production in
DTH, but not IH subjects (p = 0.003 (IL-5),
p = 0.024 (IL-10)), with no significant difference
in IFN-
levels between the two groups. In cultures from IH
responders, no IL-5 was measurable after stimulation with P6 and P7 (as
well as P5); this region of the molecule was shown previously to
stimulate markedly reduced T cell proliferation in these individuals.
Repeat proliferation assays confirmed no change in the pattern of
peptide recognition after
20 mo in IH or DTH subjects. We conclude
that T cell repertoires associated with distinct immune responses to
Tri r 2 can be distinguished based on Th2 cytokine induction by
DTH-associated major epitopes localizing to the amino-terminal region
of the molecule.
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