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J Biol Chem, Vol. 273, Issue 19, 11505-11513, May 8, 1998
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From the Stimulation of the T cell antigen receptor (TCR)
triggers a complex series of signaling events that culminate in T cell
activation and proliferation. The complex structure of the TCR has
hindered efforts to link specific signaling events induced by TCR
cross-linkage to downstream activation responses, such as interleukin-2
(IL-2) gene transcription. Previous studies have shown that the
polyomavirus-derived oncoprotein, middle T antigen (mT), transforms
rodent fibroblasts by interacting with and activating several
cytoplasmic signaling proteins (Src kinases, phospholipase C
(PLC)- Division of Oncology Research and Department
of Immunology, Mayo Clinic, Rochester, Minnesota 55905 and the
¶ Department of Metabolic Medicine, Imperial College School of
Medicine, Hammersmith Hospital Campus, Du Cane Road,
London W12 0NN, United Kingdom
1, Shc, and phosphoinositide 3-kinase (PI3-K) implicated in
cell growth control. In this study, we demonstrate that expression of
mT activates Jurkat T cells, as measured by increases in IL-2 promoter-
and NFAT (nuclear factor of activated T cells)-dependent
reporter gene transcription. The transcriptional response provoked by
mT was blocked by the immunosuppressive drug FK506, a potent inhibitor
of TCR-mediated IL-2 gene expression. Mutations that disrupted the
binding of mT to Src kinases or PLC-1 abrogated the ability of mT to
deliver the signals needed for IL-2 promoter activation. In contrast, a
mT mutant that failed to bind PI3-K induced a markedly elevated
transcriptional response in Jurkat cells, whereas mutation of the Shc
binding site in mT had little effect on the transactivating potential
of this viral oncoprotein. Additional studies demonstrated that the
association of mT with PLC-1 was necessary and sufficient to
activate both Ca2+- and Ras-dependent
signaling cascades in Jurkat cells. These results indicate that
PLC-1 activation plays pivotal and pleiotropic roles in the
stimulation of IL-2 gene expression, whereas activation of PI3-K
negatively modulates this response in Jurkat T cells.
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