A limited set of SH2 domains binds BCR through a high-affinity phosphotyrosine-independent interaction.

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Mol Cell Biol. 1992 November; 12(11): 5087-5093

A limited set of SH2 domains binds BCR through a high-affinity phosphotyrosine-independent interaction.

A J Muller, A M Pendergast, M H Havlik, L Puil, T Pawson and O N Witte

Department of Microbiology and Molecular Genetics, University of California, Los Angeles 90024.

ABSTRACT

SH2 (src homology region 2) domains are implicated in protein-proteininteractions involved in signal transduction pathways. IsolatedSH2 domains bind proteins that are tyrosine phosphorylated.A novel, phosphotyrosine-independent binding interaction betweenBCR, the Philadelphia chromosome breakpoint cluster region geneproduct, and the SH2 domain of its translocation partner c-ABLhas recently been reported. We have examined the ability ofadditional SH2 domains to bind phosphotyrosine-free BCR andcompared this with their ability to bind tyrosine-phosphorylatedc-ABL 1b. Of 11 individual SH2 domains examined, 8 exhibitedrelatively high affinity for c-ABL 1b, whereas only 4 exhibitedrelatively high affinity for BCR. Binding of tyrosine-phosphorylatedc-ABL 1b by the relatively high-affinity ABL and ARG SH2 domainswas quantitatively analyzed, and equilibrium dissociation constantsfor both interactions were estimated to be in the range of 5x 10(-7) M. The ABL SH2 domain exhibited relatively high affinityfor phosphotyrosine-free BCR as well; however, this interactionappears to be about two orders of magnitude weaker than bindingof tyrosine-phosphorylated c-ABL 1b. The ARG SH2 domain exhibitedrelatively weak affinity for BCR and was determined to bindabout 10-fold less strongly than the ABL SH2 domain. The ABLand ARG SH2 domains differ by only 10 of 91 amino acids, andthe substitution of ABL-specific amino acids into either theamino- or carboxy-terminal half of the ARG SH2 domain was foundto increase its affinity for BCR. We discuss these results interms of a model which has been proposed for peptide bindingby class I histocompatibility glycoproteins.

Mol Cell Biol. 1992 November; 12(11): 5087-5093

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