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Interleukin 27 negatively regulates the
development of interleukin 17-producing T helper cells
during chronic inflammation of the central nervous system |
Stumhofer JS, Laurence A, Wilson EH, Huang E, Tato CM,
Johnson LM, Villarino AV, Huang Q, Yoshimura A, Sehy D, Saris
CJ, O'Shea JJ, Hennighausen L, Ernst M and Hunter CA. (2006)
Nature Immunology 7:937-945.
Studies have focused on the events that influence the development
of interleukin 17 (IL-17)-producing T helper cells (T(H)-17
cells) associated with autoimmunity, such as experimental
autoimmune encephalitis, but relatively little is known about
the cytokines
that antagonize T(H)-17 cell effector responses. Here we
show that IL-27 receptor-deficient mice chronically infected
with
Toxoplasma gondii developed severe neuroinflammation that
was CD4(+) T cell dependent and was associated with a prominent
IL-17 response. In vitro, treatment of naive primary T cells
with IL-27 suppressed the development T(H)-17 cells induced
by IL-6 and transforming growth factor-beta, which was dependent
on the intracellular signaling molecule STAT1 but was independent
of inhibition of IL-6 signaling mediated by the suppressor
protein SOCS3. Thus IL-27, a potent inhibitor of T(H)-17
cell
development, may be a useful target for treating inflammatory
diseases mediated by these cells.
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