Binding of a high affinity phosphotyrosyl peptide to the Src SH2 domain: Crystal structures of the complexed and peptide-free forms

Gabriel Waksman; Steven E. Shoelson; Nalin Pant; David Cowburn; John Kuriyan

doi:10.1016/0092-8674(93)90405-F

Binding of a high affinity phosphotyrosyl peptide to the Src SH2 domain: Crystal structures of the complexed and peptide-free forms

Gabriel Waksman, Steven E. Shoelson, Nalin Pant, David Cowburn, John Kuriyan

Research output: Contribution to journal › Article › peer-review

707 Scopus citations

Abstract

The crystal structure of the Src SH2 domain complexed with a high affinity 11-residue phosphopeptide has been determined at 2.7 Å resolution by X-ray diffraction. The peptide binds in an extended conformation and makes primary interactions with the SH2 domain at six central residues: PQ(pY)EEI. The phosphotyrosine and the isoleucine are tightly bound by two well-defined pockets on the protein surface, resulting in a complex that resembles a two-pronged plug engaging a two-holed socket. The glutamate residues are in solvent-exposed environments in the vicinity of basic side chains of the SH2 domain, and the two N-terminal residues cap the phosphotyrosine-binding site. The crystal structure of Src SH2 in the absence of peptide has been determined at 2.5 Å resolution, and comparison with the structure of the high affinity complex reveals only localized and relatively small changes.

Original language	English (US)
Pages (from-to)	779-790
Number of pages	12
Journal	Cell
Volume	72
Issue number	5
DOIs	https://doi.org/10.1016/0092-8674(93)90405-F
State	Published - Mar 12 1993
Externally published	Yes

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

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10.1016/0092-8674(93)90405-F

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@article{f07babfee2ef404c82a6970b38815b3b,

title = "Binding of a high affinity phosphotyrosyl peptide to the Src SH2 domain: Crystal structures of the complexed and peptide-free forms",

abstract = "The crystal structure of the Src SH2 domain complexed with a high affinity 11-residue phosphopeptide has been determined at 2.7 {\AA} resolution by X-ray diffraction. The peptide binds in an extended conformation and makes primary interactions with the SH2 domain at six central residues: PQ(pY)EEI. The phosphotyrosine and the isoleucine are tightly bound by two well-defined pockets on the protein surface, resulting in a complex that resembles a two-pronged plug engaging a two-holed socket. The glutamate residues are in solvent-exposed environments in the vicinity of basic side chains of the SH2 domain, and the two N-terminal residues cap the phosphotyrosine-binding site. The crystal structure of Src SH2 in the absence of peptide has been determined at 2.5 {\AA} resolution, and comparison with the structure of the high affinity complex reveals only localized and relatively small changes.",

author = "Gabriel Waksman and Shoelson, {Steven E.} and Nalin Pant and David Cowburn and John Kuriyan",

note = "Funding Information: We thank L. C. Cantley, M. Eck, and S. C. Harrison for sharing data and insights prior to publication, D. Baltimore, S. K. Burley, and H. Hanafusa for helpful discussions, G. A. Petskofor suggesting the combination of MIR and molecular replacement, and K. L. Clark and J. L. Kim for assistance with DENZO, which was kindly provided by Z. Otwinowski. We are grateful to G. D. Booker and I. 0. Campbell for providing the p85 atomic coordinates. This work was supported in part by grants from the National Institutes of Health (D. C., J. K., and S. E. S.), the National Science Foundation (S. E. S.), and the Pew Foundation (J. K.).",

year = "1993",

month = mar,

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doi = "10.1016/0092-8674(93)90405-F",

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T1 - Binding of a high affinity phosphotyrosyl peptide to the Src SH2 domain

T2 - Crystal structures of the complexed and peptide-free forms

AU - Waksman, Gabriel

AU - Shoelson, Steven E.

AU - Pant, Nalin

AU - Cowburn, David

AU - Kuriyan, John

N1 - Funding Information: We thank L. C. Cantley, M. Eck, and S. C. Harrison for sharing data and insights prior to publication, D. Baltimore, S. K. Burley, and H. Hanafusa for helpful discussions, G. A. Petskofor suggesting the combination of MIR and molecular replacement, and K. L. Clark and J. L. Kim for assistance with DENZO, which was kindly provided by Z. Otwinowski. We are grateful to G. D. Booker and I. 0. Campbell for providing the p85 atomic coordinates. This work was supported in part by grants from the National Institutes of Health (D. C., J. K., and S. E. S.), the National Science Foundation (S. E. S.), and the Pew Foundation (J. K.).

PY - 1993/3/12

Y1 - 1993/3/12

N2 - The crystal structure of the Src SH2 domain complexed with a high affinity 11-residue phosphopeptide has been determined at 2.7 Å resolution by X-ray diffraction. The peptide binds in an extended conformation and makes primary interactions with the SH2 domain at six central residues: PQ(pY)EEI. The phosphotyrosine and the isoleucine are tightly bound by two well-defined pockets on the protein surface, resulting in a complex that resembles a two-pronged plug engaging a two-holed socket. The glutamate residues are in solvent-exposed environments in the vicinity of basic side chains of the SH2 domain, and the two N-terminal residues cap the phosphotyrosine-binding site. The crystal structure of Src SH2 in the absence of peptide has been determined at 2.5 Å resolution, and comparison with the structure of the high affinity complex reveals only localized and relatively small changes.

AB - The crystal structure of the Src SH2 domain complexed with a high affinity 11-residue phosphopeptide has been determined at 2.7 Å resolution by X-ray diffraction. The peptide binds in an extended conformation and makes primary interactions with the SH2 domain at six central residues: PQ(pY)EEI. The phosphotyrosine and the isoleucine are tightly bound by two well-defined pockets on the protein surface, resulting in a complex that resembles a two-pronged plug engaging a two-holed socket. The glutamate residues are in solvent-exposed environments in the vicinity of basic side chains of the SH2 domain, and the two N-terminal residues cap the phosphotyrosine-binding site. The crystal structure of Src SH2 in the absence of peptide has been determined at 2.5 Å resolution, and comparison with the structure of the high affinity complex reveals only localized and relatively small changes.

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Binding of a high affinity phosphotyrosyl peptide to the Src SH2 domain: Crystal structures of the complexed and peptide-free forms

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