T-lymphocyte interleukin 2-dependent tyrosine protein kinase signal transduction involves the activation of p56lck

  1. I D Horak,
  2. R E Gress,
  3. P J Lucas,
  4. E M Horak,
  5. T A Waldmann, and
  6. J B Bolen
  1. Laboratory of Tumor Virus Biology, National Cancer Institute, Bethesda, MD 20892.

Abstract

Addition of interleukin 2 (IL-2) to IL-2-dependent T cells results in tyrosine protein kinase signal transduction events even though the IL-2 receptor alpha and beta chains lack intrinsic enzymatic activity. Here we report that addition of IL-2 to IL-2-dependent human T cells transiently stimulates the specific activity of p56lck, a member of the src family of nonreceptor tyrosine protein kinases expressed at high levels in T lymphocytes. The ability of IL-2 to induce p56lck activation was found to be independent of the capacity of p56lck to associate with either CD4 or CD8. Following IL-2 treatment, p56lck was found to undergo serine/threonine phosphorylation modifications that resulted in altered mobility of the lck gene product on polyacrylamide gels. These observations raise the possibility that p56lck participates in IL-2-mediated signal transduction events in T cells.

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  1. PNAS March 1, 1991 vol. 88 no. 5 1996-2000
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