Association of p59fyn with the T Lymphocyte Costimulatory Receptor CD2: BINDING OF THE Fyn Src HOMOLOGY (SH) 3 DOMAIN IS REGULATED BY THE Fyn SH2 DOMAIN

Huamao Lin,Jill E Hutchcroft,Christopher E Andoniou,Malek Kamoun,Hamid Band,Barbara E Bierer

doi:10.1074/jbc.273.31.19914

Abstract

Human CD2 is a 50-55-kDa cell surface receptor specifically expressed on the surface of T lymphocytes and NK cells. Stimulation of human peripheral blood T cells with mitogenic pairs of anti-CD2 monoclonal antibodies (mAbs) is sufficient to induce interleukin-2 production and T cell proliferation in the absence of an antigen-specific signal through the T cell receptor. CD2 has been shown previously to associate physically with the Src family protein-tyrosine kinases p56(lck) and p59(fyn). We now report that stimulation of T cells with mitogenic pairs of anti-CD2 mAbs enhanced the association of the Fyn polypeptide with the CD2 complex, whereas stimulation with single anti-CD2 mAb had minimal effect. Using glutathione S-transferase (GST) fusion proteins, we found that CD2 bound to the Src homology (SH) 3 domain of Fyn. Interestingly, the CD2-Fyn association was negatively regulated by the Fyn SH2 domain; CD2 bound poorly to GST fusion proteins expressing both the SH2 and SH3 domains of Fyn. However, the inhibitory effect of the Fyn SH2 domain on binding of the Fyn SH3 domain to CD2 was relieved by peptides containing a phosphorylated YEEI sequence that bound directly to the Fyn SH2 domain. In addition, we found that the ability of the Fyn SH2 domain to precipitate tyrosine-phosphorylated proteins, including the CD3zeta chain, was enhanced after T cell stimulation with mitogenic pairs of CD2 mAbs. Finally, overexpression of a mutated Fyn molecule, in which the ability of the Fyn SH2 domain to bind phosphotyrosine-containing proteins was abrogated, inhibited CD2-induced transcriptional activation of the nuclear factor of activated T cells (NFAT), suggesting a functional involvement of the Fyn SH2 domain in CD2-induced T cell signaling. We thus propose that stimulation through the CD2 receptor leads to the tyrosine phosphorylation of intracellular proteins, including CD3zeta itself, which in turn bind to the Fyn-SH2 domain, allowing the direct association of the Fyn SH3 domain with CD2 and the initiation of downstream signaling events.

Highlights

Human CD2 is a 50 –55-kDa cell surface receptor expressed on the surface of T lymphocytes and NK cells
We report that stimulation of T cells with mitogenic pairs of anti-CD2 monoclonal antibodies (mAbs) enhanced the association of the Fyn polypeptide with the CD2 complex, whereas stimulation with single anti-CD2 mAb had minimal effect
Stimulation with Mitogenic Pairs of Anti-CD2 mAbs Increased the Association of CD2 with Phosphorylated Lck and Fyn—The Src family tyrosine kinases Lck and Fyn have been shown to associate with CD2 [21], yet how these key proteins are regulated in CD2-dependent signaling events remains to be established

Summary

Introduction

Human CD2 is a 50 –55-kDa cell surface receptor expressed on the surface of T lymphocytes and NK cells. The binding of the Fyn SH2 domain to tyrosine-phosphorylated proteins, including CD3␨ chains, was enhanced after stimulation with mitogenic combinations of anti-CD2 mAbs. we demonstrated that overexpression of a Fyn loss-of-function SH2 domain mutant, but not wild-type Fyn or a Fyn loss-of-function SH3 domain mutant, inhibited CD2-induced NFAT transcriptional activity.

Results

Conclusion