Induction of interleukin‐2 transcription by the hamster polyomavirus middle T antigen: a role for Fyn in T cell signal transduction

L Brizuela, ET Ulug, MA Jones… - European journal of …, 1995 - Wiley Online Library
L Brizuela, ET Ulug, MA Jones, SA Courtneidge
European journal of immunology, 1995Wiley Online Library
The transforming protein of mouse polyomavirus, the mouse middle T antigen (MomT), and
its counterpart in the hamster polyomavirus, the hamster middle T antigen (HamT), interact
with a number of cellular proteins. Among these are members of the Src family of tyrosine
kinases, the phosphatidylinositol 3‐kinase, the serine/threonine phosphatase PP2A and the
adaptor protein Shc (in the case of MomT). However, both the relative affinity of these
antigens for the members of the Src family and the tumor profile induced by their respective …
Abstract
The transforming protein of mouse polyomavirus, the mouse middle T antigen (MomT), and its counterpart in the hamster polyomavirus, the hamster middle T antigen (HamT), interact with a number of cellular proteins. Among these are members of the Src family of tyrosine kinases, the phosphatidylinositol 3‐kinase, the serine/threonine phosphatase PP2A and the adaptor protein Shc (in the case of MomT). However, both the relative affinity of these antigens for the members of the Src family and the tumor profile induced by their respective viruses are quite distinct. Particularly noteworthy are the preferential binding of Fyn by HamT and the induction of lymphoid malignancies by the hamster polyomavirus. Here we report that, when expressed in fibroblasts, HamT also associated with phospholipase Cγ (PLCγ), which led to an increased intracellular concentration of inositol‐1, 4, 5‐trisphosphate. We also show that expression of HamT in the mouse T cell line EL4 was sufficient to induce transcription from interleukin‐2 (IL‐2), NFAT and NFxB reporter constructs. The immunosuppressant FK506 as well as dominant negative alleles of Ras and Raf inhibited HamT‐induced IL‐2 transcription. This, together with the observation of NFAT responses, suggests that the action of HamT depended at least in part on the integrity of signal transduction pathways elicited by activated PLCγ. Furthermore, dominant negative Fyn but not the equivalent allele of Lck blocked HamT activation of IL‐2 transcription, while both Lck and Fyn dominant negative alleles blocked LT cell receptor‐mediated IL‐2 transcriptional activation. These results support the hypothesis that Fyn is involved in signal transduction events leading to IL‐2 transcriptional activation in T cells. Finally, the activation of IL‐2 transcription by HamT and not by MomT shown here parallels the ability of the hamster polyomavirus to induce lymphoid malignancies.
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