Alternative p38 activation pathway mediated by T cell receptor-proximal tyrosine kinases

Author:

Salvador, J. M.

Mittelstadt, P. R.

Guszczynski, T.

Copeland, T. D.

Yamaguchi, H.

Appella, E.

Fornace, A. J.

Ashwell, J. D.
Author Address

Ashwell, JD, NCI, Lab Immune Cell Biol, NIH, Bethesda, MD 20892 USA NCI, Lab Immune Cell Biol, NIH, Bethesda, MD 20892 USA. NCI, Gene Response Sect, NIH, Bethesda, MD 20892 USA. NCI, Lab Prot Dynam & Signaling, Frederick, MD 21702 USA. NCI, Cell Biol Lab, NIH, Bethesda, MD 20892 USA.

Abstract:

Signaling-responsive MAP kinases (MAPKs) are key in mediating immune responses and are activated through the phosphorylation of a Thr-X-Tyr motif by upstream MAPK kinases. Here we show that T cells stimulated through the T cell receptor (TCR) used an alternative mechanism in which p38 was phosphorylated on Tyr323 and subsequently autophosphorylated residues Thr180 and Tyr182. This required the TCR-proximal tyrosine kinase Zap70 but not the adaptor protein LAT, which was required for activation of extracellular signal - regulated protein kinase MAPKs. TCR activation of p38 lacking Tyr323 was diminished, and blocking of p38 activity prevented p38 dual phosphorylation in normal T cells but not in B cells. Thus, phosphorylation of Tyr323 dependent on the tyrosine kinase Lck and mediated by Zap70 serves as an important mechanism for TCR activation of p38 in T cells

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