Direct binding of Grb2 SH3 domain to FGFR2 regulates SHP2 function

Zamal Ahmed; Roger George; Chi Chuan Lin; Kin Man Suen; James A. Levitt; Klaus Suhling; John E. Ladbury

doi:10.1016/j.cellsig.2009.08.011

Direct binding of Grb2 SH3 domain to FGFR2 regulates SHP2 function

Zamal Ahmed, Roger George, Chi Chuan Lin, Kin Man Suen, James A. Levitt, Klaus Suhling, John E. Ladbury

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

31 Scopus citations

Abstract

The adaptor protein Grb2 is recruited to intracellular early signalling complexes of many receptor tyrosine kinases and plays an important role transducing signals leading to MAP kinase activation. To date the SH2 domain of Grb2 has been shown to mediate receptor interactions with phosphorylated tyrosine residues sited directly on the receptor or on auxiliary docking proteins. Here we report that FGFR2 recruits Grb2 through its C-terminal SH3 domain. The binding site of this domain was mapped to the proline-rich C-terminus of the receptor. Deletion of the last 10 amino acids of FGFR2 abrogates interaction with Grb2. Synthetic peptides based on the C-terminus of FGFR2 bind to full length Grb2 with low micromolar affinity. The function of this novel mode of Grb2 binding provides resistance to site-specific Shp2-mediated receptor dephosphorylation.

Original language	English (US)
Pages (from-to)	23-33
Number of pages	11
Journal	Cellular Signalling
Volume	22
Issue number	1
DOIs	https://doi.org/10.1016/j.cellsig.2009.08.011
State	Published - Jan 2010

Keywords

Cancer
FLIM
FRS2
Intracellular signalling
Shp2
Tyrosine kinase

ASJC Scopus subject areas

Cell Biology

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10.1016/j.cellsig.2009.08.011

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title = "Direct binding of Grb2 SH3 domain to FGFR2 regulates SHP2 function",

abstract = "The adaptor protein Grb2 is recruited to intracellular early signalling complexes of many receptor tyrosine kinases and plays an important role transducing signals leading to MAP kinase activation. To date the SH2 domain of Grb2 has been shown to mediate receptor interactions with phosphorylated tyrosine residues sited directly on the receptor or on auxiliary docking proteins. Here we report that FGFR2 recruits Grb2 through its C-terminal SH3 domain. The binding site of this domain was mapped to the proline-rich C-terminus of the receptor. Deletion of the last 10 amino acids of FGFR2 abrogates interaction with Grb2. Synthetic peptides based on the C-terminus of FGFR2 bind to full length Grb2 with low micromolar affinity. The function of this novel mode of Grb2 binding provides resistance to site-specific Shp2-mediated receptor dephosphorylation.",

keywords = "Cancer, FLIM, FRS2, Intracellular signalling, Shp2, Tyrosine kinase",

author = "Zamal Ahmed and Roger George and Lin, {Chi Chuan} and Suen, {Kin Man} and Levitt, {James A.} and Klaus Suhling and Ladbury, {John E.}",

note = "Funding Information: This work was supported by the Wellcome Trust .",

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doi = "10.1016/j.cellsig.2009.08.011",

language = "English (US)",

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AU - Ahmed, Zamal

AU - George, Roger

AU - Lin, Chi Chuan

AU - Suen, Kin Man

AU - Levitt, James A.

AU - Suhling, Klaus

AU - Ladbury, John E.

N1 - Funding Information: This work was supported by the Wellcome Trust .

PY - 2010/1

Y1 - 2010/1

N2 - The adaptor protein Grb2 is recruited to intracellular early signalling complexes of many receptor tyrosine kinases and plays an important role transducing signals leading to MAP kinase activation. To date the SH2 domain of Grb2 has been shown to mediate receptor interactions with phosphorylated tyrosine residues sited directly on the receptor or on auxiliary docking proteins. Here we report that FGFR2 recruits Grb2 through its C-terminal SH3 domain. The binding site of this domain was mapped to the proline-rich C-terminus of the receptor. Deletion of the last 10 amino acids of FGFR2 abrogates interaction with Grb2. Synthetic peptides based on the C-terminus of FGFR2 bind to full length Grb2 with low micromolar affinity. The function of this novel mode of Grb2 binding provides resistance to site-specific Shp2-mediated receptor dephosphorylation.

AB - The adaptor protein Grb2 is recruited to intracellular early signalling complexes of many receptor tyrosine kinases and plays an important role transducing signals leading to MAP kinase activation. To date the SH2 domain of Grb2 has been shown to mediate receptor interactions with phosphorylated tyrosine residues sited directly on the receptor or on auxiliary docking proteins. Here we report that FGFR2 recruits Grb2 through its C-terminal SH3 domain. The binding site of this domain was mapped to the proline-rich C-terminus of the receptor. Deletion of the last 10 amino acids of FGFR2 abrogates interaction with Grb2. Synthetic peptides based on the C-terminus of FGFR2 bind to full length Grb2 with low micromolar affinity. The function of this novel mode of Grb2 binding provides resistance to site-specific Shp2-mediated receptor dephosphorylation.

KW - Cancer

KW - FLIM

KW - FRS2

KW - Intracellular signalling

KW - Shp2

KW - Tyrosine kinase

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JO - Cellular Signalling

JF - Cellular Signalling

IS - 1

ER -

Direct binding of Grb2 SH3 domain to FGFR2 regulates SHP2 function

Abstract

Keywords

ASJC Scopus subject areas

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