Competition between Grb2 and Plcγ1 for FGFR2 regulates basal phospholipase activity and invasion

Zahra Timsah; Zamal Ahmed; Chi Chuan Lin; Fernando A. Melo; Loren J. Stagg; Paul G. Leonard; Prince Jeyabal; Jonathan Berrout; Roger G. O'Neil; Mikhail Bogdanov; John E. Ladbury

doi:10.1038/nsmb.2752

Competition between Grb2 and Plcγ1 for FGFR2 regulates basal phospholipase activity and invasion

Zahra Timsah, Zamal Ahmed, Chi Chuan Lin, Fernando A. Melo, Loren J. Stagg, Paul G. Leonard, Prince Jeyabal, Jonathan Berrout, Roger G. O'Neil, Mikhail Bogdanov, John E. Ladbury

Genomic Medicine

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

41 Scopus citations

Abstract

FGFR2-expressing human cancer cells with low concentrations of the adaptor protein Grb2 show high prevalence for metastatic outcome. In nonstimulated cells, the SH3 domain (and not the SH2 domains) of Plcγ1 directly competes for a binding site at the very C terminus of FGFR2 with the C-terminal SH3 domain of Grb2. Reduction of Grb2 concentration permits Plcγ1 access to the receptor. Recruitment of Plcγ1 in this way is sufficient to upregulate phospholipase activity. This results in elevated phosphatidylinositol 4,5-bisphosphate turnover and intracellular calcium levels, thus leading to increased cell motility and promotion of cell-invasive behavior in the absence of extracellular receptor stimulation. Therefore, metastatic outcome can be dictated by the constitutive competition between Grb2 and Plcγ1 for the phosphorylation-independent binding site on FGFR2.

Original language	English (US)
Pages (from-to)	180-188
Number of pages	9
Journal	Nature Structural and Molecular Biology
Volume	21
Issue number	2
DOIs	https://doi.org/10.1038/nsmb.2752
State	Published - Feb 2014

ASJC Scopus subject areas

Structural Biology
Molecular Biology

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@article{a525bde41c5a4c99b12621b14ac98298,

title = "Competition between Grb2 and Plcγ1 for FGFR2 regulates basal phospholipase activity and invasion",

abstract = "FGFR2-expressing human cancer cells with low concentrations of the adaptor protein Grb2 show high prevalence for metastatic outcome. In nonstimulated cells, the SH3 domain (and not the SH2 domains) of Plcγ1 directly competes for a binding site at the very C terminus of FGFR2 with the C-terminal SH3 domain of Grb2. Reduction of Grb2 concentration permits Plcγ1 access to the receptor. Recruitment of Plcγ1 in this way is sufficient to upregulate phospholipase activity. This results in elevated phosphatidylinositol 4,5-bisphosphate turnover and intracellular calcium levels, thus leading to increased cell motility and promotion of cell-invasive behavior in the absence of extracellular receptor stimulation. Therefore, metastatic outcome can be dictated by the constitutive competition between Grb2 and Plcγ1 for the phosphorylation-independent binding site on FGFR2.",

author = "Zahra Timsah and Zamal Ahmed and Lin, {Chi Chuan} and Melo, {Fernando A.} and Stagg, {Loren J.} and Leonard, {Paul G.} and Prince Jeyabal and Jonathan Berrout and O'Neil, {Roger G.} and Mikhail Bogdanov and Ladbury, {John E.}",

note = "Funding Information: J.E.L. is funded by the G. Harold and Leila Y. Mathers Charitable Foundation. R.G.O. is funded through US National Institutes of Health DK070950. We thank H. Xin for assistance with Figure 1. Full-length HA-Plcγ1 was a generous gift from J. Sondek (University of North Carolina School of Medicine).",

year = "2014",

month = feb,

doi = "10.1038/nsmb.2752",

language = "English (US)",

volume = "21",

pages = "180--188",

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T1 - Competition between Grb2 and Plcγ1 for FGFR2 regulates basal phospholipase activity and invasion

AU - Timsah, Zahra

AU - Ahmed, Zamal

AU - Lin, Chi Chuan

AU - Melo, Fernando A.

AU - Stagg, Loren J.

AU - Leonard, Paul G.

AU - Jeyabal, Prince

AU - Berrout, Jonathan

AU - O'Neil, Roger G.

AU - Bogdanov, Mikhail

AU - Ladbury, John E.

N1 - Funding Information: J.E.L. is funded by the G. Harold and Leila Y. Mathers Charitable Foundation. R.G.O. is funded through US National Institutes of Health DK070950. We thank H. Xin for assistance with Figure 1. Full-length HA-Plcγ1 was a generous gift from J. Sondek (University of North Carolina School of Medicine).

PY - 2014/2

Y1 - 2014/2

N2 - FGFR2-expressing human cancer cells with low concentrations of the adaptor protein Grb2 show high prevalence for metastatic outcome. In nonstimulated cells, the SH3 domain (and not the SH2 domains) of Plcγ1 directly competes for a binding site at the very C terminus of FGFR2 with the C-terminal SH3 domain of Grb2. Reduction of Grb2 concentration permits Plcγ1 access to the receptor. Recruitment of Plcγ1 in this way is sufficient to upregulate phospholipase activity. This results in elevated phosphatidylinositol 4,5-bisphosphate turnover and intracellular calcium levels, thus leading to increased cell motility and promotion of cell-invasive behavior in the absence of extracellular receptor stimulation. Therefore, metastatic outcome can be dictated by the constitutive competition between Grb2 and Plcγ1 for the phosphorylation-independent binding site on FGFR2.

AB - FGFR2-expressing human cancer cells with low concentrations of the adaptor protein Grb2 show high prevalence for metastatic outcome. In nonstimulated cells, the SH3 domain (and not the SH2 domains) of Plcγ1 directly competes for a binding site at the very C terminus of FGFR2 with the C-terminal SH3 domain of Grb2. Reduction of Grb2 concentration permits Plcγ1 access to the receptor. Recruitment of Plcγ1 in this way is sufficient to upregulate phospholipase activity. This results in elevated phosphatidylinositol 4,5-bisphosphate turnover and intracellular calcium levels, thus leading to increased cell motility and promotion of cell-invasive behavior in the absence of extracellular receptor stimulation. Therefore, metastatic outcome can be dictated by the constitutive competition between Grb2 and Plcγ1 for the phosphorylation-independent binding site on FGFR2.

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Competition between Grb2 and Plcγ1 for FGFR2 regulates basal phospholipase activity and invasion

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