Copyright information:Taken from "Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation"http://www.biomedcentral.com/1472-6807/7/58BMC Structural Biology 2007;7():58-58.Published online 25 Sep 2007PMCID:PMC2131756.ture elements present in the Grb7 SH2 structure as determined by WHATIF [71] are shaded from purple at the N-terminus to red at the C-terminus. Secondary structure elements of the canonical SH2 domain as defined by Eck . [41] are shown in green and orange symbols above the sequences. The boundaries of these elements differ slightly from that observed in the Grb7 SH2 domain. Residue number is for the Grb7 SH2 domain (b) Cartoon representation of the Grb7 SH2 domain shaded from purple at the N-terminus to red at the C-terminus. The extended DE loop distinguishes this family of SH2 domains from others. (c) A structural comparison of the Grb7 SH2 domain (green) with the Grb7 SH2 domain bound to an ErbB2 derived phosphopeptide (1MW4; black; [29]). The location of the bound phosphopeptide is indicated

Corrine J Porter (37413)

David N Krag (37420)

Jacqueline A Wilce (37422)

Jacqueline M Matthews (37414)

Jason W Schmidberger (37417)

Joel P Mackay (37415)

Matthew CJ Wilce (37421)

Peter J Leedman (37418)

Sharon E Pursglove (37416)

Stephanie C Pero (37419)

Dutch

Nederpel, W.A.C.

Wageningen Yield 

Bemestingsproef met stikstof en met kali : resultaten van de derde teelt chrysanten (1973)

Copyright information:Taken from "Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation"http://www.biomedcentral.com/1472-6807/7/58BMC Structural Biology 2007;7():58-58.Published online 25 Sep 2007PMCID:PMC2131756.l is coloured blue and negatively charged electrostatic potential is coloured red. The positions of the phosphate binding pocket is indicated. (b) A 2F- Felectron density map depicting the phosphate binding pocket of Grb7 SH2. A sulphate ion co-crystallised in this pocket in all four molecules in the asymmetric unit. The map is contoured at 1 σ. R438, R458, Q461 and S460 form direct contacts with the sulphate ion and are labeled. The side-chain of R462 lacks well defined density and is probably fairly mobile in the crystal

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Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation-1

Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation-7

Copyright information:Taken from "Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation"http://www.biomedcentral.com/1472-6807/7/58BMC Structural Biology 2007;7():58-58.Published online 25 Sep 2007PMCID:PMC2131756.ion of 36 μM. The data collected at 14,000 rpm (), 16,600 rpm (), 24,300 rpm () and 28,800 rpm () were fitted simultaneously using the nonlinear regression program [48]. (b) Absorbance at 280 nm verses radius data at sedimentation equilibrium for Grb7 at an initial loading concentrations of 12 μM. The data collected at 10,000 rpm () and 11,800 rpm () were fitted simultaneously using the nonlinear regression program NONLIN [77]. The represents the calculated fit to a monomer-dimer model. The residuals of the fit are shown in the . Samples were in 50 mM MES pH 6.6, 100 mM NaCl and 1 mM DTT. The experiments were conducted at 20°C

Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation-3

Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation-0

Copyright information:Taken from "Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation"http://www.biomedcentral.com/1472-6807/7/58BMC Structural Biology 2007;7():58-58.Published online 25 Sep 2007PMCID:PMC2131756.8NATE (red). The insert shows changes to signals in the boxed region of the HSQC spectrum over the course of the titration. The ratio of G7-18NATE to Grb7 SH2 is 0:1, 1:4, 1:2, 3:4, 1:1 and 2:1 in the black, red, blue, orange, purple and green spectra respectively. (b) The rate of change of peak volume over the titration series versus Grb7 SH2 domain residue number. The broken line indicates the mean rate of change. Residues that exhibited rates of change greater than this value are coloured according to their location in the Grb7 SH2 domain structure. (c) Surface representation of the Grb7 SH2 domain with residues affected by G7-18NATE binding coloured. The majority of residues cluster onto either the phosphopeptide binding surface (red) or the dimerisation interface (green). Residues shown in blue were also affected by G7-18NATE binding but do not cluster on one surface. The two images are related by a 90° rotation about the horizontal axis of the page

Grb7 SH2 domain structure and interactions with a cyclic peptide inhibitor of cancer cell migration and proliferation-5

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Bemestingsproef met stikstof en met kali : resultaten van de derde teelt chrysanten (1973)

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