Requirement for Shc in TCR-mediated activation of a T cell hybridoma

Joanne C. Pratt, Marcel R.M. Van Den Brink, Vivien E. Igras, Scott F. Walk, Kodimangalam S. Ravichandran, Steven J. Burakoff

Research output: Contribution to journalArticlepeer-review

26 Scopus citations

Abstract

Engagement of the TCR determines the fate of T cells to activate their functional programs, proliferate, or undergo apoptosis. The intracellular signal transduction pathways that dictate the specific outcome of receptor engagement have only been partially elucidated. The adapter protein, Shc, is involved in cytokine production, mitogenesis, transformation, and apoptosis in different cell systems. We found that Shc becomes phosphorylated on tyrosine residues upon stimulation of the TCR in DO11.10 hybridoma T cells; therefore, we investigated the role of Shc in activation-induced cell death in these cells by creating a series of stably transfected cell lines. Expression of Shc-SH2 (the SH2 domain of Shc) or Shc-Y239/240F (full-length Shc in which tyrosines 239 and 240 have been mutated to phenylalanine) resulted in the inhibition of activation-induced cell death and Fas ligand upregulation after TCR cross-linking. Expression of wild-type Shc or Shc- Y317F had no significant effect. In addition, we found that Shc-SH2 and Shc- Y239/240F, but not Shc-Y317F, inhibited phosphorylation of extracellular signal-regulated protein kinase and production of IL-2 after TCR cross- linking. These results indicate an important role for Shc in the early signaling events that lead to activation-induced cell death and IL-2 production after TCR activation.

Original languageEnglish
Pages (from-to)2586-2591
Number of pages6
JournalJournal of Immunology
Volume163
Issue number5
StatePublished - Sep 1 1999

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