Identification of a STAT4 binding site in the interleukin-12 receptor required for signaling

Abstract

The specificity of the various STAT SH2 domains for different tyrosine- containing peptides enables cytokines to activate different signaling pathways and to induce distinct patterns of gene expression. We show that STAT4 has a unique peptide specificity and binds to the peptide sequence pYLPSNID (where pY represents phosphotyrosine). This motif is found at tyrosine residue 800 in the β2 subunit of the interleukin-12 receptor and is required for DNA binding and transcriptional activity of STAT4. Our data demonstrate that transfection of interleukin-12 receptor β1 and β2 subunits is sufficient for STAT4 activation but not for STAT1 or STAT3 activation.