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Volume 271,
Number 1,
Issue of January 5, 1996 pp. 264-269
©1996 by The American Society for Biochemistry and Molecular Biology, Inc.
Affinity,
Specificity, and Kinetics of the Interaction of the SHC Phosphotyrosine
Binding Domain with Asparagine-X-X-Phosphotyrosine
Motifs of Growth Factor Receptors
(Received for publication, July 18, 1995; and in revised form, October 25, 1995)
Axel A.
Laminet ,
Gerald
Apell,
Leah
Conroy,
W.
Michael
Kavanaugh
The phosphotyrosine binding (PTB) domain specifically binds to
tyrosine-phosphorylated proteins, but differs in structure and
mechanism of action from the SH2 domain family. We quantitated the
affinity, specificity, and kinetics of the interaction of the SHC PTB
domain with a sequence motif, asparagine-X-X-phosphotyrosine
(NXX(pY)), found in several receptor tyrosine kinases and
oncogenic proteins. PTB domain-mediated interaction with the
NXX(pY) motif of c-ErbB2 was characterized by similar overall
affinity but slower kinetics than that reported for SH2 domains. This
suggested that unlike SH2 domains, PTB domains may not rapidly exchange
among associated proteins. Furthermore, when directly and
quantitatively compared, PTB domain binding specificity did not
significantly overlap with a panel of seven SH2 domains. Thus,
signaling pathways involving PTB and SH2 domain-mediated interactions
can be regulated separately. Finally, our data define the minimal SHC
PTB domain binding motif as NXX(pY), not NPX(pY) as
suggested by other authors, and suggest a high affinity motif,
hydrophobic residue-(D/E)-N-X-X-pY-(W/F), found in the Trk and
ErbB receptor tyrosine kinase families. We conclude that PTB domains
mediate specific protein-protein interactions independent from those
mediated by SH2 domains.

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Copyright © 1996 by the American Society for Biochemistry and Molecular Biology.
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